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Cleavage‐stage versus blastocyst‐stage embryo transfer in assisted reproductive technology

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Background

Advances in embryo culture media have led to a shift in in vitro fertilisation (IVF) practice from cleavage‐stage embryo transfer to blastocyst‐stage embryo transfer. The rationale for blastocyst‐stage transfer is to improve both uterine and embryonic synchronicity and enable self selection of viable embryos, thus resulting in better live birth rates.

Objectives

To determine whether blastocyst‐stage (day 5 to 6) embryo transfer improves the live birth rate (LBR) per fresh transfer, and other associated outcomes, compared with cleavage‐stage (day 2 to 3) embryo transfer.

Search methods

We searched the Cochrane Gynaecology and Fertility Group Specialised Register of controlled trials, CENTRAL, MEDLINE, Embase, PsycINFO, and CINAHL, from inception to October 2021. We also searched registers of ongoing trials and the reference lists of studies retrieved.

Selection criteria

We included randomised controlled trials (RCTs) which compared the effectiveness of IVF with blastocyst‐stage embryo transfer versus IVF with cleavage‐stage embryo transfer.

Data collection and analysis

We used standard methodological procedures recommended by Cochrane. Our primary outcomes were LBR per fresh transfer and cumulative clinical pregnancy rates (cCPR). Secondary outcomes were clinical pregnancy rate (CPR), multiple pregnancy, high‐order multiple pregnancy, miscarriage (all following first embryo transfer), failure to transfer embryos, and whether supernumerary embryos were frozen for transfer at a later date (frozen‐thawed embryo transfer). We assessed the overall quality of the evidence for the main comparisons using GRADE methods.

Main results

We included 32 RCTs (5821 couples or women).

The live birth rate following fresh transfer was higher in the blastocyst‐stage transfer group (odds ratio (OR) 1.27, 95% confidence interval (CI) 1.06 to 1.51; I2 = 53%; 15 studies, 2219 women; low‐quality evidence). This suggests that if 31% of women achieve live birth after fresh cleavage‐stage transfer, between 32% and 41% would do so after fresh blastocyst‐stage transfer.

We are uncertain whether blastocyst‐stage transfer improves the cCPR. A post hoc analysis showed that vitrification could increase the cCPR. This is an interesting finding that warrants further investigation when more studies using vitrification are published.

The CPR was also higher in the blastocyst‐stage transfer group, following fresh transfer (OR 1.25, 95% CI 1.12 to 1.39; I2 = 51%; 32 studies, 5821 women; moderate‐quality evidence). This suggests that if 39% of women achieve a clinical pregnancy after fresh cleavage‐stage transfer, between 42% and 47% will probably do so after fresh blastocyst‐stage transfer.

We are uncertain whether blastocyst‐stage transfer increases multiple pregnancy (OR 1.05, 95% CI 0.83 to 1.33; I2 = 30%; 19 studies, 3019 women; low‐quality evidence) or miscarriage rates (OR 1.12, 95% CI 0.90 to 1.38; I2 = 24%; 22 studies, 4208 women; low‐quality evidence). This suggests that if 9% of women have a multiple pregnancy after fresh cleavage‐stage transfer, between 8% and 12% would do so after fresh blastocyst‐stage transfer. However, a sensitivity analysis restricted only to studies with low or 'some concerns' for risk of bias, in the subgroup of equal number of embryos transferred, showed that blastocyst transfer probably increases the multiple pregnancy rate.

Embryo freezing rates (when there are frozen supernumerary embryos for transfer at a later date) were lower in the blastocyst‐stage transfer group (OR 0.48, 95% CI 0.40 to 0.57; I2 = 84%; 14 studies, 2292 women; low‐quality evidence). This suggests that if 60% of women have embryos frozen after cleavage‐stage transfer, between 37% and 46% would do so after blastocyst‐stage transfer.

Failure to transfer any embryos was higher in the blastocyst transfer group (OR 2.50, 95% CI 1.76 to 3.55; I2 = 36%; 17 studies, 2577 women; moderate‐quality evidence). This suggests that if 1% of women have no embryos transferred in planned fresh cleavage‐stage transfer, between 2% and 4% probably have no embryos transferred in planned fresh blastocyst‐stage transfer.

The evidence was of low quality for most outcomes. The main limitations were serious imprecision and serious risk of bias, associated with failure to describe acceptable methods of randomisation.

Authors' conclusions

There is low‐quality evidence for live birth and moderate‐quality evidence for clinical pregnancy that fresh blastocyst‐stage transfer is associated with higher rates of both than fresh cleavage‐stage transfer. We are uncertain whether blastocyst‐stage transfer improves the cCPR derived from fresh and frozen‐thawed cycles following a single oocyte retrieval. Although there is a benefit favouring blastocyst‐stage transfer in fresh cycles, more evidence is needed to know whether the stage of transfer impacts on cumulative live birth and pregnancy rates. Future RCTs should report rates of live birth, cumulative live birth, and miscarriage. They should also evaluate women with a poor prognosis to enable those undergoing assisted reproductive technology (ART) and service providers to make well‐informed decisions on the best treatment option available.

PICO

Population
Intervention
Comparison
Outcome

El uso y la enseñanza del modelo PICO están muy extendidos en el ámbito de la atención sanitaria basada en la evidencia para formular preguntas y estrategias de búsqueda y para caracterizar estudios o metanálisis clínicos. PICO son las siglas en inglés de cuatro posibles componentes de una pregunta de investigación: paciente, población o problema; intervención; comparación; desenlace (outcome).

Para saber más sobre el uso del modelo PICO, puede consultar el Manual Cochrane.

When trying to have a baby through assisted conception, is it better to transfer the embryo to the womb on day 3 or day 5?

Background

Many women and couples are unlikely to get pregnant and have a baby without medical treatment, due to infertility. Doctors have developed a variety of assisted reproductive technologies (ARTs), such as in vitro fertilisation (IVF), which involve the manipulation of eggs and sperm outside a woman's body, to try to increase her chances of getting pregnant.

Typically, in assisted conception, doctors collect eggs from a woman and fertilise them in a laboratory, leading to the formation of embryos. An embryo is the early stage of human development. Doctors commonly transfer one or several embryos into a woman’s womb (uterus) at one of two stages of embryo development: either the cleavage stage, which is 2 or 3 days after egg collection when an embryo typically consists of between 2 and 128 cells; or the blastocyst stage, which is 5 or 6 days after egg collection when an embryo consists of between 70 and 100 cells.

Until recently, doctors usually transferred embryos at the earlier, cleavage, stage. However, there has been a trend to transferring embryos at the later, blastocyst, stage. Researchers believe that only those embryos capable of surviving make it to the blastocyst stage; in other words, viable embryos will self‐select. So, it is thought that transferring embryos at the later stage may improve a woman's chances of becoming pregnant and having a healthy baby.

Review question

We wanted to find out if transferring embryos into a woman's womb at cleavage stage (day 2 to 3) or blastocyst stage (day 5 to 6) is better, in terms of:

– number of babies born alive (live birth rate) following embryo transfers using only 'fresh' embryos; that is, embryos that have not been frozen and subsequently thawed;

– total number of pregnancies achieved following embryo transfers using both 'fresh' and frozen then thawed embryos, collected from a single egg collection procedure (cumulative clinical pregnancy rate);

– multiple pregnancy rate (when a woman is carrying more than one baby at a time);

‐ miscarriage rate (the loss of a pregnancy before the 20th week of development in the womb).

Study characteristics

We included 32 randomised controlled trials (studies in which participants are assigned randomly to 2 or more treatment groups), which included 5821 women or couples. The evidence is current to October 2021.

Key results

– Transferring 'fresh' embryos at the blastocyst stage (day 5 to 6) may lead to more live births than when 'fresh' embryos are transferred at the cleavage stage (day 2 to 3). This suggests that if 31% of women achieve live birth after 'fresh' cleavage‐stage embryo transfer, between 32% and 41% would do so after 'fresh' blastocyst‐stage transfer.

– Transferring 'fresh' embryos at the blastocyst stage probably leads to more clinical pregnancies – defined as evidence of fetal heart activity on an ultrasound scan – than when 'fresh' embryos are transferred at the cleavage stage. This suggests that if 39% of women achieve a clinical pregnancy after 'fresh' cleavage‐stage transfer, between 42% and 47% will probably do so after 'fresh' blastocyst‐stage transfer.

– We are uncertain whether blastocyst‐stage transfer favors cumulative clinical pregnancy rates (i.e. pregnancies from both fresh and thawed cycles deriving from a single egg collection procedure).

– We are uncertain whether blastocyst‐stage transfer increases multiple pregnancy rates compared to cleavage‐stage transfer, when we consider all the studies that reported information on this.

– When we consider evidence only from higher‐quality studies and studies that transferred the same number of embryos in both embryo stages, we found that multiple pregnancy rate is probably higher in the blastocyst‐stage transfer group.

– We are uncertain whether blastocyst‐stage transfer increases miscarriage rates compared to cleavage‐stage transfer.

Future studies should report rates of live birth, cumulative live birth, and miscarriage, to enable women, couples and their doctors to make well‐informed decisions on the best treatment option available.

Quality of the evidence

We have low to moderate confidence in the quality of the evidence for most outcomes. The main limitation was the failure of some studies to describe acceptable methods of assigning women or couples at random to treatment groups.

Authors' conclusions

Implications for practice

There is low‐quality evidence that blastocyst‐stage transfer, in comparison to cleavage‐stage transfer, is associated with higher rates of live birth, and moderate‐quality evidence showing that clinical pregnancy rate is also higher in blastocyst‐stage transfer. We are uncertain whether blastocyst‐stage transfer improves the cumulative pregnancy rate (derived from fresh and thawed cycles). Given that the embryo freezing rate may be higher in cleavage‐stage transfer, more evidence about cumulative pregnancy rate and a cost‐effectiveness analysis are needed to draw firmer conclusions. Finally, there is low‐quality evidence showing that the addition of a time‐lapse system (TLS) to a cleavage‐stage transfer is still less effective than a blastocyst‐stage transfer without TLS in terms of pregnancy rate.

Implications for research

Although this review provides evidence that there is a significant difference in live birth rates from fresh cycles in favour of blastocyst‐stage transfer compared to cleavage‐stage transfer cycles, the findings for cumulative clinical pregnancy rates (derived from fresh and thawed cycles) still raise questions. Further new studies of blastocyst cycles must report live birth, cumulative live birth rates (especially when vitrification is used), and miscarriage rates to enable consumers and service providers to make well‐informed decisions on the best treatment option. Also, more studies evaluating poor prognosis women will help to obtain more information about this specific subgroup. Finally, more studies with single‐embryo transfer are also needed in order to identify the best option with the fewest adverse event rates.

Based on the results of this review, we recommend the following to ensure valuable data are produced.

  • Adherence to Consolidated Standards of Reporting Trials (CONSORT) recommendations for randomised controlled trials (RCTs), especially methods of concealment (Begg 1996).

  • Research into the best participant selection and inclusion criteria; consider prognostic factors such as age and outcomes from previous cycles.

  • Same media composition and brand for both groups up to the cleavage stage.

  • Explicit prespecified embryo transfer policies for both groups; preferably single‐embryo transfer.

  • Long‐term follow‐up reports of cumulative live birth rates (including embryo thaws) presented as a survival analysis. A minimum of a one‐year time period after randomisation for follow‐up of cumulative live birth rates within studies (as part of study protocol), and a possible follow‐up of results of transfers outside this time window in a later report (if applicable, i.e. if not all transfers have been performed within one year).

  • Research into improved blastocyst cryopreservation techniques, e.g. vitrification.

  • Reporting of miscarriage, live birth, and cumulative pregnancy rates.

Summary of findings

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Summary of findings 1. Blastocyst‐stage versus cleavage‐stage embryo transfer for assisted reproductive technology

Blastocyst‐stage versus cleavage‐stage embryo transfer for assisted reproductive technology

Population: women and couples with subfertility
Settings: assisted reproductive technology
Intervention: blastocyst‐stage embryo transfer
Comparison: cleavage‐stage embryo transfer

Outcomes per couple

Illustrative comparative risks* (95% CI)

Relative effect
(95% CI)

No. of participants
(studies)

Quality of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Cleavage‐stage embryo transfer

Blastocyst‐stage embryo transfer

Live birth rate per fresh transfer

312 per 1000

365 per 1000

(324 to 406)

OR 1.27
(1.06 to 1.51)

2219

(15 studies)

⊕⊕⊝⊝
Lowa,c

When sensitivity analysis restricted to 9 studies with low or some concerns of overall risk of bias, it results in a similar effect (OR 1.26, 95% CI 1.04 to 1.54).

Cumulative pregnancy rate (slow freezing)

565 per 1000

472 per 1000

(384 to 562)

OR 0.69

(0.48 to 0.99)

512

(4 studies)

⊕⊕⊝⊝
Lowa,c

Cumulative pregnancy rate (vitrification)

333 per 1000

550 per 1000

(369 to 719)

OR 2.44

(1.17 to 5.12)

120

(1 study)

⊕⊕⊕⊝ Moderatea

Clinical pregnancy rate

390 per 1000

444 per 1000
(417 to 470)

OR 1.25
(1.12 to 1.39)

5821
(32 studies)

⊕⊕⊝⊝
Moderatea

When sensitivity analysis restricted to 17 studies with low risk or some concerns of overall risk of bias, it results in a similar effect (OR 1.24, 95% CI 1.08 to 1.41).

Multiple pregnancy rate

89 per 1000

99 per 1000
(81 to 119)

OR 1.12
(0.90 to 1.38)

4208
(22 studies)

⊕⊕⊝⊝
Lowa,b,c

When sensitivity analysis restricted to 15 studies with low risk or some concerns of overall risk of bias, it results in an increase of multiple pregnancy rate (OR 1.33, 95% CI 1.04 to 1.70).

Miscarriage rate

67 per 1000

82 per 1000
(68 to 111)

OR 1.24, (0.98 to 1.57)

4106
(21 studies)

⊕⊕⊝⊝
Lowa,c

Embryo freezing rate

594 per 1000

412 per 1000

(369 to 455)

OR 0.48

(0.40 to 0.57)

2292

(14 studies)

⊕⊕⊝⊝
Lowa,b

I2 = 84%. Direction of effect largely consistent

Failure rate to transfer any embryos

11 per 1000

26 per 1000

(19 to 37)

OR 2.50

(1.76 to 3.55)

2577

(17 studies)

⊕⊕⊕⊝
Moderatea

I2 = 36%

*The basis for the assumed risk is the median control group risk across studies. The corresponding risk (and its 95% confidence interval) is based on the assumed risk in the comparison group and the relative effect of the intervention (and its 95% CI).
CI: confidence interval; OR: odds ratio

GRADE Working Group grades of evidence
High quality: further research is very unlikely to change our confidence in the estimate of effect.
Moderate quality: further research is likely to have an important impact on our confidence in the estimate of effect and may change the estimate.
Low quality: further research is very likely to have an important impact on our confidence in the estimate of effect and is likely to change the estimate.
Very low quality: we are very uncertain about the estimate.

aDowngraded one level for serious risk of bias: most studies have some concerns of overall risk of bias, mainly due to the randomisation process, deviations from the intended intervention and selective reporting
bDowngraded one level for serious inconsistency
cDowngraded one level for serious imprecision: findings compatible with benefit or minimal effect

Background

Description of the condition

Worldwide, 15% of reproductive‐aged couples are affected by infertility (WHO 2022). The World Health Organization estimates that, globally, between 48 million couples and 186 million individuals live with infertility (WHO 2021). Assisted reproductive technologies (ARTs), such as in vitro fertilisation (IVF), intracytoplasmic sperm injection (ICSI), and embryo freezing, are considered beneficial for many couples and women who are unlikely to conceive without treatment, and for whom less invasive forms of treatment have failed or are unlikely to be effective. The fledgling era of IVF, from 1980 to the mid‐1990s, was characterised by relatively static successful pregnancy rates of around 20%. The past decade, however, has given rise to advances in ovarian stimulation, cell culture, embryo transfer, and new cryopreservation techniques as well as freeze‐all cycles, that have culminated in significant overall improvements in successful pregnancies (Wirleitner 2016; Roque 2015). This is evident in the annual statistical reports from different areas of the globe. One such report, for example, has demonstrated a doubling of the pregnancy rate per embryo transfer cycle from 1994 to 2003, despite a decrease in the mean number of embryos transferred (Waters 2006).

Description of the intervention

IVF involves the use of hormones to stimulate the ovaries to produce many eggs (oocytes), followed by egg collection (oocyte retrieval), addition or injection of sperm, fertilisation, embryo culture, and lastly, the return of a few selected embryos to the uterus (embryo transfer).

Conventionally, embryos have been transferred on either day 2 or day 3 when the embryos were two to eight cells, or 'cleavage stage', because the uterus was thought to provide the best environment for the survival of the embryo (Laverge 2001). The question of optimal timing for embryo transfer arises when examining the differences between IVF procedures and what happens naturally in vivo. Day 2 is an early time at which morphological grading of the embryos is possible, allowing selection of the 'best' embryos for transfer. Embryo morphology, along with other factors, is thought to be highly indicative of pregnancy outcome (De Placido 2002). Early replacement in the uterus may be advantageous for the embryos by limiting the time spent in the in vitro environment of the embryology laboratory.

Over the past decade, there has been a steady shift in practice to the transfer of embryos on day 5 or 6, when the embryos are 'blastocysts'. With the introduction of a variety of commercial preparations of sequential media in the late 1990s, the ART service sector witnessed an explosion of worldwide interest in blastocyst culture, with most clinics conducting research into its application in their own settings. As a result, a substantial volume of publications followed. These documented trials with conflicting results and reflected debates about the merits and drawbacks of extended culture (Sfontouris 2021; Sunde 2016; Sunde 2021).

One of the benefits of blastocyst‐stage transfer could be the potential for an improved implantation rate, which could lead to a change in policy about the number of embryos to be transferred (Kamath 2020). The higher the implantation rate is, the lower the number of embryos are transferred.

The fact that many blastocyst‐stage transfer trials were not prospectively randomised or were underpowered has contributed to the lack of a strong consensus about best practice for blastocyst culture. The need for an evidence‐based approach using meta‐analysis of small trials was, therefore, required to assist in deciphering the overall effect of blastocyst culture to help identify participant subsets and practices that might best benefit from this approach.

How the intervention might work

Blastocyst culture is not novel; indeed, the very first report of an IVF pregnancy was from a transferred blastocyst (Edwards 1995). Despite this, cleavage‐stage transfer was adopted as standard global practice early in the history of IVF for two reasons: the low developmental rate of embryos cultured past this stage; and the observation that, unlike other primates, human embryos have an unusual propensity to survive when replaced prematurely into the uterus (Marston 1977). However, as knowledge of embryo metabolic requirements expanded, so did the range of more advanced culture media (Scholtes 1996), and co‐culture techniques, culturing endometrial cells in co‐culture with the embryo (Menezo 1990; Van Blerkom 1993; Yeung 1992). One important finding was that the in vitro environment in which a cleavage‐stage embryo grows best is different from that for a blastocyst. This led to the evolution of stage‐specific (or sequential) media (G1/G2) by Gardner in 1998 (Gardner 1998b): embryos are transferred on day 3 from a medium containing low concentrations of glucose and one or more amino acids to a medium containing higher concentrations of glucose and a wider range of amino acids (Gardner 1996). At this stage, the embryo undergoes cell compaction and genomic activation so that the embryo is no longer under the control of transcripts and ribonucleic acid (RNA) messages of maternal origin (Braude 1998). With the application of stage‐specific media, there have been reports of blastocyst development rates as high as 60% to 65% (Schoolcraft 2001). Interestingly, with the development of time‐lapse systems (TLS), stage‐specific media is no longer considered essential (Armstrong 2019). Time‐lapse systems take frequent digital images of embryos, allowing embryologists to assess their quality without physically removing them from the incubator.

There are two central arguments why blastocyst culture has possible advantages over traditional cleavage‐stage transfer. Firstly, it is considered to be physiologically premature to expose early‐stage embryos to the uterine environment, particularly one that has been subjected to superovulation and thus high levels of oestrogen (Valbuena 2001). In vivo, embryos travel through the fallopian tubes and do not reach the uterus before the morula (16‐cell compacted) stage (Croxatto 1972), which equates to at least day 4 of in vitro culture. The uterus provides a different nutritional environment from the oviduct. Therefore, it is postulated that the uterine environment may cause stress on the embryo, if transferred at cleavage stage (Baart 2006; Munne 2002), and result in reduced implantation potential (Fanchin 2001; Gardner 1996).

The second argument for blastocyst‐stage transfer is the reported higher implantation potential compared with cleavage‐stage embryos. As a consequence of self selection, it is postulated that only the most viable embryos are expected to develop into blastocysts. It is widely acknowledged that the morphological criteria used for selection of the best embryos on day 2 to 3 are limited. Many published studies that debate the correlation of morphological features with pregnancy rates can be found in the literature (Palmstierna 1998; Puissant 1987; Roseboom 1995; Scott 2000; Sjoblom 2006; Steer 1992). It is now understood that a disturbingly large proportion of morphologically‐normal day 3 embryos are chromosomally abnormal or mosaic, thus contributing to the 80% to 90% rate of implantation failure post‐transfer that is observed in cleavage‐stage protocols (Magli 1998). While the transfer of day 5 blastocysts cannot ensure the absence of chromosomal abnormality (Magli 2000), Staessen 2004 demonstrated that, at least in women older than 36 years, the incidence can be reduced from 59% in day 3 embryos to 35% in day 5 blastocysts. The question that this review aims to answer is whether the higher implantation rates do translate into higher live birth rates.

Arguments against blastocyst culture are largely related to this process of self selection. Women undergoing blastocyst culture are expected to have a higher incidence of cycle cancellation due to failed embryo development (Marek 1999), and to have fewer embryos cryopreserved (frozen) (Tsirigotis 1998).

Overall utilisation rates have previously been described as the total number of embryos transferred plus the embryos thawed divided by the number of fertilised eggs. Whilst this approach presents information about the comparative number of pregnancy opportunities that each treatment approach can provide a woman or couple, it does not take into account the implantation potential for fresh and thawed embryos. Cumulative live birth rate is the only outcome that can assess this. An alternative efficacy formula was developed in the Schoolcraft 2001 study that does take cumulative pregnancy rate into account. Using the formula (mean number of embryos transferred multiplied by implantation rate) plus (mean number of embryos cryopreserved multiplied by implantation rate) minus (1 minus cancellation rate), this group of researchers was able to demonstrate a 19% greater efficiency in blastocyst culture compared to cleavage‐stage transfers. Disappointingly, such a utilisation and efficiency analysis is not possible in the majority of RCTs due to the lack of reporting of frozen‐thawed cycle outcomes within a reasonable time frame for trials. A frozen‐thawed cycle is an embryo transfer that is performed at a later date with embryos that were frozen a few days after the oocyte retrieval. We would argue that a superior approach to both of the foregoing methods is to report the live birth rates for both fresh and frozen‐thawed cycles following a single oocyte retrieval in women randomised to either cleavage‐stage or blastocyst‐stage transfers.

Why it is important to do this review

This is an update of a Cochrane Review first published in 2002, and previously updated in 2005, 2007, 2012, and 2016.

Advocates of blastocyst culture are confident that only the most viable embryos survive the extended culture to day 5 or 6. They argue that this results in a higher probability of implantation and requires fewer embryos to be transferred, thereby lowering the costly multiple birth rate (Gardner 1998b; Jones 1999). It is important to be aware that clinic policies may differ on the minimum criteria for blastocyst culture and the day on which this decision is made (for example, number of follicles, fertilised eggs, 8‐cell embryos on day 3) (Milki 1999). It is also yet to be clarified if there are patient groups for whom blastocyst culture is disadvantageous. Most importantly, does blastocyst culture achieve the primary aim of providing the subfertile couple with a normal, healthy baby? Methods for identifying viable blastocysts are a popular research focus, involving a range of approaches which include identification of chromosomally‐normal blastocysts by polar‐body and blastomere, trophectoderm genetic analysis (using microarrays or next‐generation sequencing known as pre‐implantation genetic screening (Jones 2008)), and metabolomic analysis of culture media (Nel‐Themaat 2011).

Critics of the blastocyst culture approach express concern at the increased incidence of women failing to have embryos available for transfer (Marek 1999), although the day of participant recruitment into the blastocyst programme is crucial to this argument.Other negative outcomes reported to be associated with blastocyst culture include a higher incidence of monozygotic twinning and altered sex ratio in favour of males (Menezo 1999; Spangmose 2020). Monozygotic twinning is frequently reported at above 1% in ART cycles (Sills 2000), whilst the background rate of monozygotic twins in spontaneous conceptions is in the order of 1 in 330. This twinning is associated with miscarriage, serious structural congenital anomalies, growth discrepancy and twin‐to‐twin transfusion syndrome. Extended culture of an embryo has been implicated as one of the interventions associated with an increase in monozygotic twinning (Behr 2000; Cohen 1990; De Felici 1982; Jain 2004), but a recent report suggests that improvements in cell culture techniques over time can result in a significant decrease in its incidence (Moayeri 2007). Similarly, as the underlying mechanisms that lead to an altered sex ratio are elucidated, whether it be media constituents or simply the morphological selection criteria (Luna 2007), the imbalance may also be rectified.

The aim of this review is to determine whether the number of days between oocyte retrieval and embryo transfer (that is, the embryo stage) has any effect on the success of ART treatment, and in particular, the live birth rate, the most important outcome for couples or women undergoing treatment as well as for service providers.

Objectives

To determine whether blastocyst‐stage (day 5 to 6) embryo transfer improves the live birth rate (LBR) per fresh transfer, and other associated outcomes, compared with cleavage‐stage (day 2 to 3) embryo transfer.

Methods

Criteria for considering studies for this review

Types of studies

We included only individually‐randomised parallel‐group trials (RCTs). We excluded quasi‐RCTs and cluster‐randomised trials. We also excluded cross‐over trials unless pre‐cross‐over data were available.

Types of participants

Inclusion criteria

We included couples or women affected by subfertility undergoing in vitro fertilisation (IVF) or intracytoplasmic sperm injection (ICSI) for therapeutic reasons or for oocyte donation within all patient prognosis groups.

'Patient prognosis groups' (participant subsets or populations) is a term used to describe the categories that couples or women are assigned to based on several factors such as their age, type of subfertility, ovarian response to the superovulation drugs, and number of previous attempts. See the Subgroup analysis and investigation of heterogeneity section below for the categories.

Exclusion criteria

We excluded couples or women whose IVF or ICSI cycle, or both, involved in vitro matured oocytes or pre‐implantation genetic screening. We also excluded couples or women whose frozen‐thawed cycle results were shown, but where no data were available from the fresh cycle.

Types of interventions

Inclusion criteria

We included studies comparing blastocyst‐stage (day 5 to 6) transfers to cleavage‐stage (day 2 to 3) transfers in settings using single and sequential media culture methods for IVF and ICSI, where the embryos were grown for between 2 and 6 days in vitro prior to embryo transfer.

Exclusion criteria

We excluded studies using co‐culture methods as an intervention.

We also excluded studies comparing blastocyst‐stage transfers to cleavage‐stage transfers in frozen‐thawed cycles, but where no data were available from the fresh cycle.

Types of outcome measures

Primary outcomes

  • Live birth rate per couple or woman (number of live births after week 20 of pregnancy per couple or woman) following fresh transfer

  • Cumulative pregnancy rate (cCPR) per couple or woman (from both fresh and thawed cycles deriving from a single egg collection procedure)

Secondary outcomes

  • Clinical pregnancy rate per couple or woman: number of couples or women achieving a clinical pregnancy following fresh transfer (defined by the demonstration of foetal heart activity on ultrasound scan)

  • Multiple pregnancy rate per couple or woman following fresh transfer: number of multiple pregnancies per couple or woman

  • High‐order multiple pregnancy rate per couple or woman following fresh transfer: three or more foetal heartbeats per couple or woman

  • Miscarriage rate for fresh transfer: number of occurrences per couple or woman and per pregnant woman

  • Embryo freezing rates per couple or woman: number of couples or women that had supernumerary embryos for transfer at a later date per couple or woman

  • Failure rate to transfer embryos (per couple or woman): percentage of couples or women that did not have an embryo transfer

Additional outcomes not appropriate for statistical pooling

We were unable to pool data per cycle or per embryo transfer or per oocyte pick up (OPU) (Vail 2003). If a study included multiple cycles, transfers, or OPUs per woman, then results reported per cycle/transfer/OPU cannot be validly pooled. If the study reported results per cycle/transfer/OPU and this did not coincide with the point of randomisation (i.e. if the denominator did not coincide with the point in the treatment where randomisation occurred), we calculated new results using randomised participants as the denominator and treated those excluded as having negative outcomes. However, due to the frequency that this form of data is reported in the literature, we have entered them into the 'Data and analyses tables' for the following outcomes.

  • Live births per OPU and embryo transfer.

  • Clinical pregnancy rate per OPU and embryo transfer.

  • Implantation rate: the number of foetal sacs divided by the number of embryos transferred.

Search methods for identification of studies

We obtained all reports that described (or might have described) RCTs comparing cleavage‐stage embryo transfer and blastocyst‐stage transfer in the treatment of subfertility, using IVF or ICSI, using the search strategy developed by the Gynaecology and Fertility Group.

Electronic searches

We searched the following databases.

  • The Cochrane Gynaecology and Fertility Group Specialised Register of Controlled Trials, searched 20 October 2021, ProCite platform (Appendix 1).

  • CENTRAL via the Cochrane Register of Studies Online (CRSO), searched 20 October 2021, Web platform (Appendix 2).

  • MEDLINE, searched from 1946 to 20 October 2021, Ovid platform (Appendix 3).

  • Embase, searched from 1980 to 20 October 2021, Ovid platform (Appendix 4).

  • PsycINFO, searched from 1806 to 20 October 2021, Ovid platform (Appendix 5).

  • CINAHL (Cumulative Index to Nursing and Allied Health Literature), searched from 1961 to 4 April 2020, EBSCO platform (Appendix 6). Any later CINAHL search output is contained in the 2021 CENTRAL search output.

We combined the MEDLINE search with the Cochrane highly sensitive search strategy for identifying randomised trials, which appears in the Cochrane Handbook for Systematic Reviews of Interventions (Higgins 2019a, hereafter referred to as the Cochrane Handbook).

We combined the Embase search with trial filters developed by the Scottish Intercollegiate Guidelines Network (SIGN) (www.sign.ac.uk/what-we-do/methodology/search-filters/). We did not impose any language restrictions in these searches.

Searching other resources

We searched the National Research Register, a register of ongoing and recently completed research projects funded by, or of interest to, the United Kingdom's National Health Service (NHS); entries from the Medical Research Council Clinical Trials Register; and details on reviews in progress that are collected by the NHS Centre for Reviews and Dissemination.

We also searched ClinicalTrials.gov and the World Health Organization (WHO) International Clinical Trials Registry Platform (ICTRP) (Appendix 7; Appendix 8).

We performed the search on titles, abstracts, and keywords of the listed articles. We also searched the citation lists of relevant publications, review articles, and included studies. We handsearched relevant conference abstracts and contacted experts in the field.

We conduct a search for new trials bi‐annually and update the review as and when we find new trials to be incorporated.

Data collection and analysis

Selection of studies

Three review authors (DG, CAS, and AQR) performed the selection of trials for inclusion in the review after employing the search strategy described previously. Two review authors independently viewed each record. We resolved any disagreements about eligibility through discussion. We have presented details of the included studies in the Characteristics of included studies tables, which provide a context for assessing the reliability of results. We have described excluded studies in the Characteristics of excluded studies table.

Data extraction and management

Two of three review authors (DG, CAS, and AQR) extracted data from eligible studies using a data extraction form designed and pilot‐tested by the authors. Two review authors independently viewed each record. We resolved any disagreements about data extraction through discussion. Data extracted included study characteristics and outcome data. Where studies had multiple publications, we used the main trial report as the primary reference and derived additional details from secondary papers. We corresponded with study investigators for further data, as required.

Assessment of risk of bias in included studies

Two of three review authors (DG, SC, and AC) independently assessed the included studies for risk of bias using the Cochrane risk of bias 2 (RoB 2) assessment tool (Higgins 2019b; Sterne 2019). We assessed: bias arising from the randomisation process; bias due to deviations from intended interventions; bias due to missing outcome data; bias in measurement of the outcome; and bias in selection of the reported result. The effect of interest was the effect of assignment to the intervention at baseline, regardless of whether the interventions were received as intended (the 'intention‐to‐treat effect').

A potential deviation from the intended protocols is an adherence issue, such as moving to the cleavage transfer arm if there were few available embryos on day 3. Another potential deviation is a difference that could be found in the number of transferred embryos in each of the arms. Although both of these deviations could occur in the real world, they could also occur as a result of participating in a trial.

The outcomes we selected to be assessed for risk of bias are the same as those reported in the summary of findings table: live birth, cumulative pregnancy, clinical pregnancy, multiple pregnancy, miscarriage, embryo freezing, and failure to transfer any embryo. We describe the measurement methods and time points in the Measures of treatment effect section.

Judgements were classified as 'low' or 'high' risk of bias, or as expressing 'some concerns', assigned as recommended in the Cochrane Handbook, Chapter 8 (Higgins 2019a). We resolved any disagreements about risk of bias judgements through discussion. We described all judgements fully and presented the consensus judgements in the main review document (e.g. as a table, or a figure, or within a forest plot of the results).

These domain‐level judgements provided the basis for an overall risk of bias judgement for the specific trial result being assessed.

We used the RoB 2 Excel tool (available on the riskofbiasinfo.org website) to process the use of RoB 2 and to store data for presentation (Sterne 2019). We made risk of bias data available by providing detailed appendices.

We sought additional information on trial methodology or actual original trial data from the principal author of trials that appeared to meet eligibility criteria but were unclear in aspects of methodology, or where the data were in a form unsuitable for meta‐analysis. We sent reminder correspondence when a reply was not received within three weeks.

Measures of treatment effect

For dichotomous data (for example, clinical pregnancy rate), we expressed results for each study as odds ratios (ORs) with 95% confidence intervals (CIs) and combined them for meta‐analysis with RevMan Web 2020 (RevMan Web 2020).

Unit of analysis issues

The primary analysis was per woman randomised. We counted multiple live births (for example, twins or triplets) as one live birth event.

Dealing with missing data

We analysed the data on an intention‐to‐treat basis as far as possible (i.e. including all randomised participants in analysis, in the groups to which they were randomised). We attempted to obtain missing data from the original trialists. Where these were unobtainable, we imputed individual values to all the outcomes: they were assumed not to have occurred in participants without a reported outcome.

Assessment of heterogeneity

We considered whether the clinical and methodological characteristics of the included studies were sufficiently similar for meta‐analysis to provide a clinically meaningful summary. We assessed statistical heterogeneity by the measure of the I2 statistic. An I2 measurement greater than 50% was taken to indicate substantial heterogeneity. When we detected substantial heterogeneity, we explored possible explanations in subgroup analyses. We took statistical heterogeneity into account when interpreting the results.

We examined heterogeneity between the results of different studies by inspecting the scatter of data points, the overlap in their confidence intervals, and more formally, by checking the results of the Chi2 tests. A priori, we had planned to look at the possible contribution of differences in trial design to the heterogeneity identified. Where possible, we pooled the outcomes statistically.

Assessment of reporting biases

In view of the difficulty of detecting and correcting for publication bias and other reporting biases, we aimed to minimise their potential impact by ensuring a comprehensive search for eligible studies and by being alert to duplication of data. If there were ten or more studies in an analysis, we used a funnel plot to explore the possibility of small study effects (a tendency for estimates of the intervention effect to be more beneficial in smaller studies).

Data synthesis

We performed statistical analyses in accordance with the Cochrane Handbook (Higgins 2019a). The primary analyses included all studies.

We pooled data for meta‐analysis with RevMan Web 2020 (RevMan Web 2020), using the fixed‐effect Mantel‐Haenszel model method. We entered the data on the graphs so that, for beneficial outcomes (for example, pregnancy), data are displayed to the right of the line of no effect, and in detrimental outcomes (for example, miscarriage), to the left of the line of no effect.

Subgroup analysis and investigation of heterogeneity

We planned the following subgroup analyses for the outcomes live birth, cumulative pregnancy, clinical pregnancy, and multiple pregnancy.

  • Studies that actively selected for good prognosis participants (for example, four or more zygotes, first two cycles, more than 10 follicles, young population, no male‐factor individuals) versus participants with poor prognostic factors (for example, previous failed ART cycles or poor response to ovulation stimulation) versus studies with unselected participants.

  • Studies that randomised at the start of the cycle (that is, prior to ovarian stimulation) were compared with those that randomised at the days immediately prior to and post‐OPU (that is, day of final ultrasound scan and prior to human chorionic gonadotropin trigger up to and including the day of fertilisation check, when numbers of oocytes are anticipated).

  • Studies where the policy for the number of embryos replaced was equal in both blastocyst‐stage and cleavage‐stage groups versus studies where fewer blastocyst‐stage than cleavage‐stage embryos were replaced.

  • We also included a post hoc analysis to investigate substantial heterogeneity for one of the primary outcomes: studies where freezing technique was slow freezing versus studies where vitrification was used.

  • We made a subgroup analysis for time‐lapse s ystem s election (TLS selection ) with algorithm which was not stated in the protocol, as TLS is a technology that was unavailable when the protocol was written. Subgroups would be:

    • Conventional cleavage stage versus conventional blastocyst stage;

    • TLS selection (with algorithm) cleavage stage versus conventional blastocyst stage;

    • TLS selection (with algorithm) cleavage stage versus TLS selection (with algorithm) blastocyst stage.

We planned to perform an overall assessment of risk of bias for subgroups.

Sensitivity analysis

Primary analysis pooled the data of all the studies. The selected outcomes assessed by a sensitivity analysis are live birth, cumulative pregnancy, clinical pregnancy, and embryo freezing.

Eligibility was restricted to studies with outcomes with 'low' or 'some concerns for' overall risk of bias.

Summary of findings and assessment of the certainty of the evidence

We prepared a summary of findings table using GRADEpro and Cochrane methods (GRADEpro GDT; Higgins 2019a). This table evaluated the overall quality of the body of evidence for the main review outcomes (live birth rate, cumulative pregnancy rate, clinical pregnancy rate, multiple pregnancy rate, miscarriage rate, embryo freezing rate and failure rate to transfer any embryos) for the main review comparison (blastocyst‐stage transfer versus cleavage‐stage transfer). We assessed the quality of the evidence using GRADE criteria: overall risk of bias (fed by RoB2 tool assessment), consistency of effect, imprecision, indirectness, and publication bias. Two review authors working independently made judgements about evidence quality (high, moderate, low, or very low), resolving any disagreements through discussion. We justified, documented, and incorporated our judgements into the reporting of results for each outcome.

We planned to extract study data, format our comparisons in data tables, and prepare a summary of findings table before writing the results and conclusions of our review.

Results

Description of studies

Results of the search

At the 2022 update we identified 1651 articles as potentially relevant for comparing blastocyst‐stage versus cleavage‐stage embryo transfer, and we retrieved 26 new articles in full text. In the 2022 update we included five new studies (Hatirnaz 2017; Kaser 2017; Levi‐Setti 2018; Singh 2017; Yang 2018), and there were 3 newly excluded studies (Cornelisse 2018; Green 2016; Holden 2017). Including studies retrieved in the latest update, we now have 32 studies (47 articles) in the review. See Figure 1.


Study flow diagram: results of search from review inception to 2020 (update of the flow diagram published in 2016)

Study flow diagram: results of search from review inception to 2020 (update of the flow diagram published in 2016)

We also found 7 new ongoing studies. In total, there are 9 ongoing studies: one each from China (ChiCTR‐ICR‐15006184), Iran (NCT01107002), and the USA (Neuhausser 2020); two from Italy (ISRCTN48090543; NCT02639000), and the Netherlands (Cornelisse 2021); and three from Egypt (NCT04210414; PACTR201402000773124; PACTR201709002592834).

We attempted to contact study authors for information regarding methodology and outcome data. We received replies from 11 contact authors (Bungum 2003; Fernandez‐Shaw 2015; Frattarelli 2003; Hreinsson 2004; Karaki 2002; Levitas 2004; Levron 2002; Livingstone 2002, Papanikolaou 2005; Papanikolaou 2006; Rienzi 2002). Cumulative live birth data were provided by Fernandez‐Shaw 2015.

Included studies

Study design and setting

We included 32 parallel‐design RCTs in this review (5821 participants). The size of trials ranged from 20 in Fisch 2007 to 460 couples or women in Kolibianakis 2004, including both comparison groups.

The majority of trials were carried out in less than six months, except for the two largest studies. All studies were reported to have been performed at single private clinics or university‐based clinics. Twelve countries were represented in the included studies, with Belgium being the most prolific, providing six studies. The countries represented were: Australia (Livingstone 2002); Belgium (Devreker 2000; Emiliani 2003; Kolibianakis 2004; Papanikolaou 2005; Papanikolaou 2006; Van der Auwera 2002); Brazil (Motta 1998); China (Yang 2018); Denmark (Bungum 2003); Egypt (Elgindy 2011; Gaafar 2015); France (Brugnon 2010); Greece (Pantos 2004); India (Kaur 2014; Singh 2017); Iran (Aziminekoo 2015); Israel (Coskun 2000; Levitas 2004; Levron 2002); Italy (Levi‐Setti 2018; Rienzi 2002; Schillaci 2002); Jordan (Karaki 2002); Spain (Fernandez‐Shaw 2015; Ten 2011); Sweden (Hreinsson 2004); Turkey (Hatirnaz 2017); and the USA (Fisch 2007; Frattarelli 2003; Gardner 1998a; Kaser 2017).

Participants

Participant selection criteria comprised three main groups: unselected participants (Emiliani 2003; Fernandez‐Shaw 2015; Gaafar 2015; Hatirnaz 2017; Karaki 2002; Kolibianakis 2004; Motta 1998; Pantos 2004; Schillaci 2002; Van der Auwera 2002); good prognostic factors where participants were positively selected; that is, those who would be expected to do well with blastocyst culture (Brugnon 2010; Bungum 2003; Coskun 2000; Elgindy 2011; Fisch 2007; Frattarelli 2003; Gardner 1998a; Hreinsson 2004; Kaser 2017; Kaur 2014; Levi‐Setti 2018; Levron 2002; Livingstone 2002; Papanikolaou 2005; Papanikolaou 2006; Rienzi 2002; Singh 2017; Ten 2011; Yang 2018); and poor prognostic factors, where couples or women were selected who had experienced multiple failures with conventional treatment or had a poor response to ovulation induction (Aziminekoo 2015; Devreker 2000; Levitas 2004). Most studies recruited women under 40 years of age, except for Fernandez‐Shaw 2015, Gardner 1998a, and Gaafar 2015, which had no age limit. The mean age across all the studies varied from 29 years to 34 years.

We found no studies of participants using donor eggs.

Interventions

Twenty trials used sequential media, of which 13 used Vitrolife G1/G2, while the remaining media were combinations of brands or made in‐house. Five did not state the media used (Table 1).

Open in table viewer
Table 1. Culture techniques of included studies

Trial

Culture technique day 2/3

Culture technique day 5/6

Aziminekoo 2015

Sydney IVF cleavage medium, Cook

Sydney IVF blastocyst medium

Brugnon 2010

G series™ medium (Vitrolife, Sweden)

G series™ medium (Vitrolife, Sweden)

Bungum 2003

Sequential G1 Vitrolife

Sequential G1/G2 Vitrolife

Coskun 2000

Sequential MediCult

Sequential G1/G2 Vitrolife

Devreker 2000

NS

NS

Elgindy 2011

NS

NS

Emiliani 2003

In‐house sequential (based on G1/G2)

In‐house sequential (based on G1/G2)

Fernandez‐Shaw 2015

Sequential G1 Vitrolife

Sequential G1/G2 Vitrolife

Fisch 2007

NS

NS

Frattarelli 2003

NS

NS

Gaafar 2015

NS

NS

Gardner 1998a

Single Ham's F10 In‐house

Sequential G1/G2 In‐house

Hatirnaz 2017

Standard culture medium

Sequential G1/G2 Scandinavian IVF Sciences

Hreinsson 2004

Vitrolife IVF

Sequential G1/G2 or CCM Vitrolife

Karaki 2002

MediCult

Sequential G1/G2 Vitrolife

Kaser 2017

Global total with HSA LifeGlobal

Global total with HSA LifeGlobal

Kaur 2014

Cleavage medium

G2 Plus media

Kolibianakis 2004

Sequential G1 Vitrolife

Sequential G1/G2 Vitrolife

Levi‐Setti 2018

NS

NS

Levitas 2004

NS

Sequential ‐ G1/G2 Vitrolife

Levron 2002

NS

NS

Livingstone 2002

Sequential ‐ Sydney IVF Cook

Sequential ‐ Sydney IVF Cook

Motta 1998

Sequential ‐ Irvines P1

Sequential ‐ Irvines P1 then Blast media

Pantos 2004

Papanikolaou 2005

Sequential ‐ Vitrolife G1/G2 GII or GIII

Sequential ‐ Vitrolife G1/G2 GII or GIII

Papanikolaou 2006

Assume sequential ‐ Vitrolife G1/G2

Assume sequential ‐ Vitrolife G1/G2

Rienzi 2002

Sequential G1 Vitrolife

Sequential G1/G2 Vitrolife

Schillaci 2002

NS

NS

Singh 2017

NS

NS

Ten 2011

NS

NS

Van der Auwera 2002

Sequential both Cook and Vitrolife

Sequential both Cook and Vitrolife

Yang 2018

Sequential media (G1.5, Vitrolife) in a Primo Vision time‐lapse system (Vitrolife)

Sequential G1/G2 Vitrolife

CCM: a Vitrolife trademarked medium for blastocyst culture
IVF: in vitro fertilisation
G1/G2:sequential media from Vitrolife
NS: not stated

Freezing of embryos in both experimental groups was reported in 14 of the 32 included trials (Brugnon 2010; Bungum 2003; Fernandez‐Shaw 2015; Gardner 1998a; Hreinsson 2004; Karaki 2002; Kolibianakis 2004; Levron 2002; Motta 1998; Pantos 2004; Papanikolaou 2006; Rienzi 2002; Ten 2011; Van der Auwera 2002). Coskun 2000 reported no provision for day 5 freezing. Levitas 2004 stated that most of the remaining embryos were not suitable for freezing. Other interventions, such as assisted hatching, were either not provided or not reported on for the majority of trials. Gardner 1998a was the only trial that practised assisted hatching, but only for the day 3 embryo transfer group.

All the studies compared blastocyst‐stage versus cleavage‐stage embryo transfers. For the cleavage‐stage transfer groups, most transfers were on day 3, except for five trials that did the embryo transfers on day 2 (Devreker 2000; Emiliani 2003; Gaafar 2015; Motta 1998; Van der Auwera 2002), and one study that had a policy of transferring on day 2 or 3 (Levitas 2004).

The trials that provided details on the ovarian stimulation regimen mostly reported using a similar gonadotropin‐releasing hormone pituitary down‐regulation protocol prior to human menopausal gonadotropin (HMG) and follicle stimulating hormone (FSH) administration. However, in some trials (Kolibianakis 2004; Levi‐Setti 2018; Papanikolaou 2005; Papanikolaou 2006; Singh 2017), gonadotropin‐releasing hormone antagonists were used in varying degrees.

Two studies (Kaser 2017; Yang 2018) evaluated the effects of adding time‐lapse system (TLS) to cleavage‐stage transfer.

Outcomes

  • 15/32 studies reported live birth rate per fresh embryo transfer

  • 5/32 studies reported cumulative pregnancy rate

  • 32/32 studies reported clinical pregnancy rate

  • 22/32 studies reported multiple pregnancy rate

  • 13/32 studies reported high‐order multiple pregnancy rate

  • 21/32 studies reported miscarriage rate

  • 14/32 studies reported embryo freezing rate (when there are supernumerary embryos for transfer at a later date)

  • 17/32 studies reported failure rate to transfer embryos

Excluded studies

We excluded 10 studies from the review for the following reasons. Six were not truly randomised studies (Cornelisse 2018; Green 2016; Holden 2017; Levron 2001; Utsonomiya 2004; Zech 2007). Three studies used co‐culture (Bungum 2002; Guerin 1991; Menezo 1992). In the remaining study, fresh embryo transfers on day 5 or 6 were not the main intervention (Loup 2009).

One study (Clua Obrado 2020) randomised Spanish recipients between 18 and 50 years old in their first or second synchronous cycle to D3 or D5 embryo transfer. The authors will not provide the missing information until its publication, therefore it awaits classification.

Risk of bias in included studies

We attempted to obtain additional information regarding all aspects of randomisation, blinding, power analysis, and intention‐to‐treat from all trial authors.

We accessed the RoB 2 tool on 20 August 2020. Risk of bias assessments for each outcome, including all domain judgements and support for the judgement, are located within each included study, and at the side of all forest plots. To access further detailed risk of bias assessment data, please use the following link.

The risk of bias judgements for outcomes across all studies were predominantly of 'some concerns' and 'high'. The most common reason for 'some concerns' of overall risk of bias was the lack of publication of the protocol in a trial registry, while overall high risk of bias was mainly due to lack of reporting of allocation concealment.

Detailed risk of bias assessment data (with consensus responses to the signalling questions) are available upon reasonable request to the authors.

Effects of interventions

See: Summary of findings 1 Blastocyst‐stage versus cleavage‐stage embryo transfer for assisted reproductive technology

Blastocyst‐stage versus cleavage‐stage transfer

For an overview of our main analyses, please see summary of findings Table 1.

Primary outcomes
1. Live birth rate per couple or woman

The live birth rate per fresh embryo transfer was higher in the fresh blastocyst transfer group (odds ratio (OR) 1.27, 95% confidence interval (CI) 1.06 to 1.51; I2 = 53%; 15 studies, 2219 women; low‐quality evidence; Analysis 1.1; Figure 2). This suggests that if 31% of women achieve live birth after fresh cleavage‐stage transfer, between 32% and 41% would do so after fresh blastocyst‐stage transfer.


Forest plot of comparison: 1 Blastocyst‐ versus cleavage‐stage transfer: live birth rate, outcome: 1.1 live birth per couple

Forest plot of comparison: 1 Blastocyst‐ versus cleavage‐stage transfer: live birth rate, outcome: 1.1 live birth per couple

Subgroup and sensitivity analyses

We did not find evidence that the treatment effect differed between fresh cleavage‐stage and blastocyst‐stage transfer based either on number of embryos transferred (test for subgroup differences: P = 0.48, I² = 0%; Analysis 1.2) or on the prognosis (test for subgroup differences: P = 0.73, I² = 0%; Analysis 1.3).

Sensitivity analysis including only those studies with low or some concerns of overall risk of bias found a higher live birth rate in the blastocyst group (OR 1.26, 95% CI 1.04 to 1.54; I2 = 69%; 9 studies, 1821 women; moderate‐quality evidence).

2. Cumulative clinical pregnancy rate per couple or woman (following fresh and frozen‐thawed transfer)

We are uncertain whether blastocyst‐stage transfer improves cumulative clinical pregnancy rate (OR 0.89, 95% CI 0.64 to 1.22; I2 = 71%; 5 studies, 632 women; very low‐quality evidence; Analysis 2.1). There was substantial heterogeneity for this outcome, with differing directions of effect. The heterogeneity was largely attributable to two studies (Fernandez‐Shaw 2015; Rienzi 2002). We investigated statistical heterogeneity by conducting a post hoc subgroup analysis according to the method of freezing. The test for subgroup differences showed a significant difference between the subgroups (Chi² = 9.12, degrees of freedom (df) = 1 (P = 0.003), I² = 89.0%). The only study using vitrification showed evidence of higher cumulative pregnancy rate in blastocyst transfers (OR 2.44, 95% CI 1.17 to 5.12; moderate‐quality evidence; Fernandez‐Shaw 2015), whilst the four studies with slow freezing showed that the confidence interval is too wide to know if blastocyst transfer decreases the cumulative pregnancy rate (OR 0.69, 95% CI 0.48 to 0.99; low‐quality evidence). This is an interesting finding which should be investigated further when more studies using vitrification are published.

Subgroup and sensitivity analyses

We did not find evidence that the treatment effect differed between fresh cleavage‐stage and blastocyst‐stage transfer based on number of embryos transferred (test for subgroup differences: P = 0.89, I² = 0%) or day of randomisation (test for subgroup differences: P = 0.42, I² = 0%), and no conclusive evidence of a difference based on prognosis (test for subgroup differences: P = 0.05, I² = 73.6%; Analysis 2.2; Analysis 2.3; Analysis 2.4).

We are also uncertain whether blastocyst‐stage transfer improves the cumulative pregnancy rate when we run a sensitivity analysis including only those studies with low or some concerns of overall risk of bias (OR 1.10, 95% CI 0.74 to 1.61; I2 = 73%; 3 studies, 427 women; very low‐quality evidence).

Secondary outcomes
3. Clinical pregnancy rate per couple or woman

The clinical pregnancy rate was higher in the fresh blastocyst‐transfer group (OR 1.25, 95% CI 1.12 to 1.39; I2 = 51%; 32 studies, 5821 women; moderate‐quality evidence; Figure 3). This suggests that if 39% of women achieve a clinical pregnancy after fresh cleavage‐stage transfer, between 42% and 47% would do so after fresh blastocyst‐stage transfer.


Forest plot of comparison: 2 Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy rate, outcome: 2.1 clinical pregnancy rate per couple

Forest plot of comparison: 2 Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy rate, outcome: 2.1 clinical pregnancy rate per couple

Subgroup and sensitivity analyses

We did not find evidence that the treatment effect differed between fresh cleavage‐stage and blastocyst‐stage transfer for clinical pregnancy rate. However, the separate analysis of subgroups shows that clinical pregnancy rate may be higher in the fresh blastocyst‐stage transfer group when the number of transferred embryos is equal (OR 1.31, 95% CI 1.16 to 1.48; I2 = 48%; 20 studies; 4434 women) and for single embryo transfers (OR 1.31, 95% CI 1.04 to 1.65; I2 = 43; 5 studies; 1241 women). We also found that good prognosis participants (OR 1.25, 95% CI 1.09 to 1.43; I2 = 51%; 9 studies, 3645 women) and unselected participants (OR 1.22, 95% CI 1.01 to 1.46; I2 = 64%; 10 studies, 1981 women) may have a higher clinical pregnancy rate if fresh embryo transfer was done at blastocyst stage. When analysing a fresh blastocyst transfer without TLS versus TLS cleavage‐stage transfer, the blastocyst transfer group also may have a higher pregnancy rate (OR 1.41, 95% CI 1.04 to 1.90; I2 =0%; 2 studies, 709 women). However, when analysing TLS blastocyst‐stage transfer versus TLS cleavage‐stage transfer, no differences were found (OR 0.91, 95% CI 0.43 to 1.96; 1 study, 110 women).

Sensitivity analysis including only those studies with low risk of bias for allocation concealment did not substantially influence our findings (OR 1.52, 95% CI 1.19 to 1.94; I2 = 68%; 8 studies, 1097 women), though heterogeneity was high. However, we found that transferring at fresh blastocyst stage had a higher clinical pregnancy rate when randomisation was done on day 2 or 3 after oocyte pick up (OPU) (OR 1.59, 95% CI 1.13 to 2.23; I2 = 63%; 4 studies, 537 women), but no differences were found when randomisation was performed earlier.

4. Multiple pregnancy rate per couple or woman

We are uncertain of the effect of the embryo stage on the multiple pregnancy rate in fresh cycles (OR 1.12, 95% CI 0.90 to 1.38; I2 = 24%; 22 studies, 4208 women; low‐quality evidence). This suggests that if 9% of women have a multiple pregnancy after fresh cleavage‐stage transfer, between 8% and 12% would do so after fresh blastocyst‐stage transfer.

Subgroup and sensitivity analyses

We did not find evidence that the treatment effect differed between fresh cleavage‐stage and blastocyst‐stage transfer based on number of embryos transferred, prognosis, or day of randomisation (Analysis 4.2; Analysis 4.3; Analysis 4.4).

Sensitivity analysis including only studies with low or some concerns of overall risk of bias showed that transferring at blastocyst stage probably increases the multiple pregnancy rate (OR 1.33, 95% CI 1.04 to 1.70; moderate‐quality evidence).

We are uncertain of the effect of the embryo stage on the high‐order multiple pregnancy rate in fresh cycles (OR 0.45, 95% CI 0.18 to 1.15; I2 = 0%; 13 studies, 2335 women).

5. Miscarriage rate for fresh transfer

We are uncertain of the effect of the embryo stage on the miscarriage rate per couple or woman in fresh cycles (OR 1.24, 95% CI 0.98 to 1.57; I2 = 0%; 21 studies, 4106 women; low‐quality evidence).

6. Embryo freezing rate per couple or woman

Rates of embryo freezing when there are supernumerary embryos for transfer at a later date per couple or woman were lower in the blastocyst transfer group (OR 0.48, 95% CI 0.40 to 0.57; I2 = 84%; 14 studies, 2292 women; low‐quality evidence). There was very high heterogeneity, but the direction of effect was consistent in most studies.

7. Failure rate to transfer embryos

Rates of failure to transfer any embryos were higher in the blastocyst transfer group (OR 2.50, 95% CI 1.76 to 3.55; I2 = 36%; 17 studies, 2577 women; moderate‐quality evidence).

8. Other data

Blastocyst formation rates

As reported in Table 2, blastocyst formation rates, which show the proportion of 2PN embryos that get to blastocyst stage (day 5 to 6 transfer only) ranged from 22.4% in Aziminekoo 2015 to 60.3% in Schillaci 2002.

Open in table viewer
Table 2. Blastocyst formation and implantation rate (in day 5 to 6 transfers)

Study

Blastocyst formation rate

Implantation D2/3

Implantation D5/6

Other

Aziminekoo 2015

22.4%

21/173; 12.1%

22/152; 14.5%

Brugnon 2010

Not stated

24/52; 46.2%

23/55; 41.8%

Bungum 2003

55.2%

50/114; 43.9%

44/120; 36.7%

2/61 participants had only 1 blastocyst

Coskun 2000

28%

50/235; 21.3%

52/218; 23.9%

77% participants had at least 1 blastocyst

Devreker 2000

Not stated

1/34; 2.9%

8/19; 42.1%

Elgindy 2011

97%

71/197; 36%

53/280; 19%

Emiliani 2003

48%

57/197; 28.9%

50/168; 29.8%

Fernandez‐Shaw 2015

67.7 %

20/71; 28.1%

36/84; 42.8%

Fisch 2007

Not stated

11/12; 92%

4/8; 50%

Frattarelli 2003

Not stated

18/69; 26.1%

23/53; 43.4%

Gaafar 2015

Not stated

Not stated

Not stated

Gardner 1998a

46.5%

64/174; 36.8%

53/95; 55.8%

85% women had at least 2 blastocysts

Hatirnaz 2017

52.6%

45/95; 47.4%

43/95; 45.3%

Hreinsson 2004

33%

29/139; 20.9%

24/114; 21.1%

2 morula replaced (one implanted). 60% pregnancy rate when top‐quality blasts transferred

Karaki 2002

33%

37/291 12.7%

37/142; 26.1%

9/80 cancelled due to lack of blastocysts (unselected)

Kaser 2017

Not stated

23/56; 41.1%

26/53; 49.1%

Kaur 2014

Not stated

66/309; 21.4%

102/290; 35.2%

Kolibianakis 2004

50.7%

96/234; 41.0%

94/226; 41.6%

Levi‐Setti 2018

Not stated

25.67%

28.37%

Levitas 2004

43%

4/56; 7.1%

10/24; 4.2%

Day 5‐7 26% cancelled due to lack of blastocysts (poor prognosis)

Levron 2002

34.2%

53/137; 38.7%

20/99; 20.2%

6.5% cancelled due to lack of blastocysts (good prognosis)

Livingstone 2002

Not stated

Motta 1998

Not stated

51/262; 19.5%

36/120; 30.0%

6/58 cycles cancelled D5 no blastocysts

Pantos 2004

44.6%

15.8%

15.8%

Papanikolaou 2005

Not stated

35/170; 20.6%

59/158; 37.3%

4/158 women had only 1 blast transferred due to lack of availability and 1 had it on request

Papanikolaou 2006

Not stated

38/156; 24%

58/149; 38.9%

Number of participants with no embryos available D3: 8 and D5: 11

Rienzi 2002

44.8%

34/96; 35.4%

38/100; 38.0%

Good prognosis

Schillaci 2002

60.3%

23/168; 13.7%

26/110; 23.6%

Unselected population nil cancellations D5

Singh 2017

Not stated

Not stated

Not stated

Ten 2011

Not stated

21/54; 38.9%

26/56; 46.4%

Good prognosis

Van der Auwera 2002

44.7%

31/106; 29.2%

41/90; 45.6%

27% cancellation D5 (unselected population)

Yang 2018

Not stated

80/290; 62.1%

22/306; 72.5%

Implantation data

For blastocyst‐stage transfer, the implantation rate varied from 4.2% to 55.8%. For cleavage‐stage transfer, the implantation rate varied from 3% to 43.9% (see Table 2).

Assessment of publication bias

We generated funnel plots for the outcomes of live birth and clinical pregnancy. They did not suggest publication bias (see Figure 4; Figure 5).


Funnel plot of comparison: 1 Blastocyst‐ versus cleavage‐stage transfer: live birth rate, outcome: 1.1 live birth per couple

Funnel plot of comparison: 1 Blastocyst‐ versus cleavage‐stage transfer: live birth rate, outcome: 1.1 live birth per couple


Funnel plot of comparison: 2 Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy rate, outcome: 2.1 clinical pregnancy rate per couple

Funnel plot of comparison: 2 Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy rate, outcome: 2.1 clinical pregnancy rate per couple

Discussion

Summary of main results

In the 15 RCTs that reported live birth rates, there was low‐quality evidence of a benefit in live birth rate per couple or woman in the fresh blastocyst transfer group and there was no evidence of a difference in the miscarriage rate. Clinical pregnancy rates were also higher in the fresh blastocyst transfer group, based on moderate‐quality evidence. When the comparator was TLS cleavage‐stage transfer, the benefit favoured blastocyst transfer as well.

We did not find any evidence of a difference when pooling the five RCTs that reported cumulative pregnancy rates (derived from fresh and thawed cycles from a single oocyte retrieval cycle): three were published in 2002/2003, one in 2010, and one in 2015. However, a post hoc analysis showed an interesting finding in which a blastocyst‐stage transfer may improve the cumulative pregnancy rate when the method of freezing was vitrification, but not when slow freezing was used (low‐quality evidence). This finding should be regarded cautiously as it resulted from a post hoc subgroup analysis.

Embryo freezing rates and failure rates to transfer embryos favoured early cleavage‐stage transfers. We did not find any evidence of a difference between fresh blastocyst‐stage and cleavage‐stage transfers for rates of miscarriage, multiple pregnancies, or high‐order multiple pregnancies.

Overall completeness and applicability of evidence

The data in this review of 32 RCTs are incomplete. Of 32 RCTs, only five reported cumulative pregnancy rates. Three of the five new studies (for the 2022 update) failed to report live birth data and all five failed to report cumulative pregnancy rates. This lack of data from the subsequent frozen‐thawed cycles and, therefore, the lack of data on cumulative pregnancy rates, means that couples and women are not adequately informed about the outcomes.

For a well‐informed decision between a cleavage‐stage or blastocyst‐stage embryo transfer policy, professionals, couples and women consider multiple variables, such as the chance of pregnancy, the time to pregnancy, the safety of the treatment, its burden, and the costs involved. The fact that the freezing rate is higher in cleavage‐stage transfer highlights the importance of getting the cumulative pregnancy rates data, in order to draw more complete conclusions (Cornelisse 2018).

The applicability of the evidence to everyday practice is somewhat limited by the many variables present in an in vitro fertilisation (IVF) cycle, which directly result from different clinic policies. Although the 32 studies all compared cleavage‐stage with blastocyst‐stage embryo transfer, they differed with respect to media used, freezing protocols, policies about the numbers of embryos transferred, the use of time‐lapse systems for embryo selection, and embryo quality scores. However, the most serious limitation was the lack of data from the frozen‐thawed cycles, as alluded to in the previous paragraph. For the most part, the variation in the different protocols can be a strength, as it means that in spite of the variation in cycles, the effect is still seen. With so few studies reporting the most useful outcome (cumulative pregnancy rate), it is difficult to report the applicability of the evidence.

Blastocyst culture is expected to result in higher implantation rates (number of fetal sacs observed divided by the number of embryos transferred). However, pooling of implantation data could not be included in the meta‐analysis as this would not generate valid estimates or confidence intervals due to the unit of analysis used (Vail 2003). Implantation rate is also no longer considered a useful outcome for a number of methodological reasons (Griesinger 2016).

There was a significantly higher failure rate to transfer any embryos in the blastocyst‐stage group, leading to cycle cancellation. The increased rates of failure to transfer with blastocyst stage is largely because of embryos with arrested development prior to the day of embryo transfer. Indeed, many of the studies that transferred fewer blastocysts than cleavage‐stage embryos did so from a lack of options rather than by policy. Only the reporting of fresh and frozen‐thawed cycle embryos can overcome this challenge. Although it could be better for some women to learn that their embryos failed to develop by day 5 than go through with a transfer at cleavage stage with embryos that had a low potential for success, there has been little research into the emotional status of couples or women given such choices (Borg 2000). Avoiding unnecessary embryo transfer needs to be balanced against the need for an additional oocyte retrieval. The possibility that extended culture may cause harm to viable embryos, through suboptimal culture conditions, must be considered, particularly when there are large variations between trials in blastocyst development rates.

There are no good‐quality studies showing the data of women with poor prognosis, such as few available embryos, or women at advanced reproductive age. Both scenarios are extremely common, yet the evidence to make an educated decision in these scenarios is still missing. We found one ongoing study Neuhausser 2020) that intends to analyse these subgroups. Thus, the next update of this review may be able to assess this information.

The varying embryo transfer policies between the two experimental groups was also a concern: a significant number of the studies had a policy to transfer fewer embryos in the blastocyst‐stage group than in the cleavage‐stage group (Table 3). There are two primary reasons for this difference. First, there is a reduced survival rate of day 5 to 6 blastocysts. Second, many clinics worried about the high incidence of multiple pregnancies with blastocysts will have a policy to transfer no more than two blastocyst‐stage embryos. Some clinics state that by employing blastocyst culture, they have been able to reduce the multiple pregnancy rate whilst maintaining the pregnancy rate. In this review, many of the studies were still transferring two to three embryos. Single‐embryo transfers for selected patient groups are now considered standard practice in many clinics throughout the world (Hamberger 2005).

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Table 3. Mean number of embryos transferred

Study ID

Day 2/3

Day 5/6

Aziminekoo 2015

2.8 ± 1.1

2.6 ± 0.6

Brugnon 2010

1.0 ± 0

1.0 ± 0

Bungum 2003

2.0 ± NS

2.0 ± NS

Coskun 2000

2.3 ± 0.6

2.2 ± 0.5

Devreker 2000

2.8 ± NS

1.7 ± NS

Elgindy 2011

2.8 ± 0.4

2.0 ± 0.2

Emiliani 2003

2.1 ± 0.4

1.9 ± 0.3

Fernandez‐Shaw 2015

1.5 ± 0.5

1.4 ± 0.5

Fisch 2007

1.0 ± 0

1.0 ± 0

Frattarelli 2003

3.0 ± 0.5

2.0 ± 0.2

Gaafar 2015

NS

NS

Gardner 1998a

3.7 ± 0.1

2.2 ± 0.1

Hatirnaz 2017

1.4 ± 0.6

1.4 ± 0.4

Hreinsson 2004

1.8 ± NS

1.9 ± NS

Karaki 2002

3.5 ± 0.6

2.0 ± 0.1

Kaser 2017

1.0 ± 0

1.0 ± 0

Kaur 2014

2.0 ± 0.7

1.9 ± 0.5

Kolibianakis 2004

1.9 ± 0.1

1.8 ± 0.1

Levi‐Setti 2018

1.9 ± 0.4

1.8 ± 0.6

Levitas 2004

3.4 ± NS

1.9 ± NS

Levron 2002

3.1 ± 0.6

2.3 ± 0.8

Livingstone 2002

2.0 ± NS

1.0 ± NS

Motta 1998

4.6 ± NS

2.3 ± NS

Pantos 2004

4.0 ± 1.5

3.4 ± 1.1

Papanikolaou 2005

2.0 ± 0

2.0 ± 0.5

Papanikolaou 2006

1.0 ± 0

1.0 ± 0

Rienzi 2002

2.0 ± 0

2.0 ± 0

Schillaci 2002

2.8

1.8

Singh 2017

NS

NS

Ten 2011

2.0 ± NS

2.0 ± NS

Van der Auwera 2002

1.9 ± 0.3

1.9 ± 0.2

Yang 2018

1.0 ± 0

1.0 ± 0

NS ‐ not stated

The importance of selecting the single most viable embryo for transfer has intensified the search to improve assessment of the quality of embryos. Performing blastocyst culture may offer one of those mechanisms (Gardner 2004; Milki 2004). In this meta‐analysis, significantly fewer embryos were transferred in the blastocyst‐stage group than in the cleavage‐stage group. When we performed a subgroup analysis for trials where equal numbers of embryos were transferred (including single‐embryo transfers), the clinical pregnancy rate remained unchanged. It could be argued that this is the most valid comparison, because trials with a greater number of cleavage‐stage embryos being transferred are probably advantaged inappropriately.

Regardless of the embryo transfer policy, for many women, there is simply a lack of choice, as only one, if any, embryo reaches the blastocyst stage. Only three studies in this review had a policy for single‐blastocyst transfer, although only one reported the live birth rate. None of the new studies added to this updated review had a single‐embryo transfer policy.

Studies have shown that women with a high oocyte yield and good‐quality 8‐cell embryos on day 3 are more likely to have blastocysts by day 5 to 6 than poor responders and those with no 8‐cell embryos by day 3. Therefore, we considered whether outcomes might be influenced by the time of randomisation. In subgroup analysis for live birth and pregnancy outcomes, we compared studies that randomised couples or women prior to the start of the treatment cycle (at a time when neither the number of oocytes retrieved nor fertilised nor the number of 8‐cell embryos could be anticipated) versus studies that randomised women at a later stage. We found no evidence of a statistically significant difference between the subgroups.

Miscarriage rates were reported in just over half of the included trials. Theoretically, the rate of miscarriage might be expected to be lowest with the transfer of highly selected embryos into a better synchronous uterine environment, such as in blastocyst culture. However, the results to date reveal little change from earlier reviews that showed no evidence of a difference in miscarriage rates for couples or women randomised (odds ratio (OR) 1.15, 95% confidence interval (CI) 0.88 to 1.50; 21 studies). Only seven of the included trials reported on the presence or absence of monozygotic twinning, so this analysis remains underpowered to comment meaningfully on monozygotic twin rates. A total of three sets of monozygotic twins were reported, two with cleavage‐stage embryo transfers and only one set of monozygotic twins from blastocyst transfer. Monozygotic twin rates in assisted reproductive technologies (ARTs) are thought to be underestimated, with up to one‐third being missed without genetic testing (Vitthala 2009).

Overall, this review found that women in the blastocyst group were less likely to have any embryos frozen, but there was no clear evidence of a difference in cumulative pregnancy rate (fresh and frozen‐thawed cycle transfers). The number of embryos frozen is an important consideration when assessing the effectiveness of a treatment, as it may offer women an additional opportunity to achieve a pregnancy. When considering an alteration in treatment procedure from cleavage‐stage to blastocyst‐stage transfer, the benefits of possible higher implantation rates are weighed up against the disadvantages of not only higher failure rates to transfer, but also lower cryopreservation rates.

Five trials reported data on pregnancies following transfer of frozen‐thawed embryos in both groups (Brugnon 2010; Emiliani 2003; Fernandez‐Shaw 2015; Rienzi 2002; Van der Auwera 2002). Van der Auwera 2002 reported a cumulative live birth rate of 47% in the blastocyst‐stage transfer group and 52% in the cleavage‐stage transfer group. That is, the added benefit of a higher cryopreservation rate in the cleavage‐stage group cancelled out the higher implantation rates of the fresh day 5 to 6 transfers. Similarly, Rienzi 2002 and Brugnon 2010 reported no evidence of a difference in cryo‐augmented pregnancy rates when at least one thawed cycle was carried out in the cleavage‐stage group. Emiliani 2003, on the other hand, reported significantly higher cumulative pregnancy rates in the cleavage‐stage group, presumably correlating to the much lower cryosurvival rate they reported in their blastocyst group (cleavage stage: 46%; blastocyst stage: 27%). However, Fernandez‐Shaw 2015 reported significantly higher cumulative pregnancy rates in the blastocyst‐stage group (day 3: 43.3%; day 5: 56.8%). This study was the only study to use vitrification, and also included women with a good prognosis. The pooled data for cumulative clinical pregnancy has 71% heterogeneity and this appears to be explained by the differences in freezing methods. This is supported by other reports of improved blastocyst outcomes with vitrification (Edgar 2012; Gardner 2003; Iwayama 2011; Richter 2016).

Although the evidence is limited, there is a growing trend for freeze‐only cycles to further reduce the risk of ovarian hyperstimulation (OHSS) and improve pregnancy outcomes if the progesterone levels are elevated (Roque 2015; Zaat 2021). This trend will also have an impact on the decision about cleavage‐stage or blastocyst‐stage transfers and should be considered in the next update.

Quality of the evidence

The overall quality of the evidence in this review was low for most outcomes and moderate for clinical pregnancy rate and failure to transfer any embryos. The main limitations in evidence quality were serious imprecision and serious risk of bias. Blinding is not possible with this intervention. Only half of the included studies adequately described their method of sequence generation, and less than one‐third reported their allocation concealment method. For some outcomes, we also downgraded the quality of evidence for imprecision. The large imprecision impacts most of the outcomes: both in cases in which we cannot say if the intervention increases or decreases the outcome rates, and also in some cases in which we cannot say if the intervention increases those rates a little or a lot.

Live birth rates were reported in 15 trials, providing low‐quality evidence (serious risk of bias and imprecision). Data for cumulative pregnancy rates after fresh and frozen‐thawed embryo transfer were only reported in five trials, in which heterogeneity was found. The most likely explanation for the heterogeneity was the difference in freezing protocols, with one study using vitrification and reporting benefit for blastocyst‐stage transfer for the cumulative pregnancy rate (Fernandez‐Shaw 2015), and the other four studies using slow freezing and reporting benefit for cleavage‐stage transfer.

Potential biases in the review process

As far as possible, we adhered to the protocol methodology in order to limit any potential biases. However, we added one new outcome – cumulative pregnancy rates (derived from fresh and thawed cycles) – in the 2016 update. This outcome reflects the policy of fresh embryo transfer and freezing remaining embryos for transfer later and more correctly reflects modern IVF practice than a single cycle transfer. Although we contacted study authors to try to obtain data for cumulative pregnancy rates, most did not collect this information.

There is an important distinction between the outcomes 'live birth rate following fresh transfer' and ‘cumulative pregnancy rate’. In the last decade, many studies only reported the outcome live birth rate following the first transfer, and trialists are generally used to reporting this outcome. Due to the extended embryo culture in blastocyst‐stage transfers, the selected embryos are potentially of higher quality, but the number available for transfer is reduced, which could potentially affect the cumulative pregnancy outcomes. Still, low‐quality evidence showed that cumulative pregnancy rate, when using vitrification, may benefit blastocyst transfer as well.

The issue of publication bias is important in systematic reviews as it may result in incorrect conclusions being reached. For example, it might be expected that the pressure for clinics to obtain high implantation rates with blastocyst culture could lead to a bias in publication towards those that do achieve this. However, the funnel plots for live birth and clinical pregnancy did not suggest publication bias.

Another point to consider is the widely varying policies for assessing minimal quality of embryos for transfer that may have existed amongst trials. Some trials accepted transfer of developmentally‐delayed embryos in blastocyst stage, whilst other trials were more selective and denied transfer of embryos that had not reached the late morula or early blastocyst stage. A strict selection policy for blastocyst transfer could have a potential bias in favor of the cleavage stage arm for two outcomes, embryo freezing rate per couple and failure rate to transfer embryos per couple. The freezing rate can be higher and the failure rate to transfer embryos lower in the cleavage stage group.

Blastocyst formation rates may also influence the pregnancy rate per embryo transfer for each trial. They ranged from 22.4% in the Aziminekoo 2015 trial to 60% in the Schillaci 2002 trial. Of the included trials that provided information on the media used, all used sequential media for the culture of blastocysts. However, while the majority reported using various versions of Vitrolife G1/G2, others used a combination of different brands, or made the media in‐house. This highlights the possibility that different brands and formulations are likely to influence the blastulation rates and subsequent outcomes. Improvements in culture media and embryo laboratory procedures should prompt new studies.

We note that there are six ongoing studies that started more than five years ago, and which have not yet published findings. These may raise a concern about publication bias.

Finally, although we took steps to conduct an exhaustive search for eligible trials, it is possible that our search strategy failed to find some studies, resulting in bias.

Agreements and disagreements with other studies or reviews

This Cochrane Review is in agreement with the Papanikolaou 2008 systematic review, which reported that cycles where equal numbers of embryos were transferred had higher live birth rates in blastocyst‐stage transfers than in cleavage‐stage tranfers. Our review also includes the cumulative pregnancy rate. Another systematic review was published by Wang 2014, which only included RCTs published after 2004. Wang 2014 shows similar results with respect to live birth rates, but reported lower miscarriage rates in the blastocyst group, which was not observed in our review. Two published reviews that cited the previous version of this review are in agreement that better studies are required (Maheshwari 2016; Martins 2016), and argue that analysing obstetric and neonatal outcomes results is critical in drawing clearer conclusions. Another systematic review by Martins 2017 emphasises that there is still too much uncertainty to conclude that transferring at one stage is better than the other.

Alviggi 2018 published a systematic review of retrospective studies, analysing perinatal outcomes. They showed that blastocyst transfers may slightly increase the preterm and very preterm birth rates but may decrease the small‐for‐gestational‐age rates in fresh cycles. However, these associations were not seen in frozen transfers.

Busnelli 2019 published a systematic review including mostly retrospective studies, analysing the risk factors for monozygotic twins. They showed that blastocyst transfer may be one of the factors to increase the risk of monozygotic twins.

Spangmose 2020 published a large retrospective cohort study analysing obstetric and perinatal outcomes, after fresh blastocyst or cleavage transfer. They showed that fresh blastocyst transfer increases the risk of placenta previa, preterm birth, and monozygotic twins. Furthermore, an altered male‐female ratio with more males following blastocyst transfer was seen.

The same study group published a large retrospective cohort study (Ginström 2019), analysing obstetric and perinatal outcomes, after frozen‐thawed transfer of vitrified blastocysts or slow‐frozen cleavage‐stage embryos. They showed a higher risk of preterm birth after blastocyst‐stage transfer. For maternal outcomes, no significant differences were found, although the precision was limited.

Study flow diagram: results of search from review inception to 2020 (update of the flow diagram published in 2016)

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Figure 1

Study flow diagram: results of search from review inception to 2020 (update of the flow diagram published in 2016)

Forest plot of comparison: 1 Blastocyst‐ versus cleavage‐stage transfer: live birth rate, outcome: 1.1 live birth per couple

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Figure 2

Forest plot of comparison: 1 Blastocyst‐ versus cleavage‐stage transfer: live birth rate, outcome: 1.1 live birth per couple

Forest plot of comparison: 2 Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy rate, outcome: 2.1 clinical pregnancy rate per couple

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Figure 3

Forest plot of comparison: 2 Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy rate, outcome: 2.1 clinical pregnancy rate per couple

Funnel plot of comparison: 1 Blastocyst‐ versus cleavage‐stage transfer: live birth rate, outcome: 1.1 live birth per couple

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Figure 4

Funnel plot of comparison: 1 Blastocyst‐ versus cleavage‐stage transfer: live birth rate, outcome: 1.1 live birth per couple

Funnel plot of comparison: 2 Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy rate, outcome: 2.1 clinical pregnancy rate per couple

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Figure 5

Funnel plot of comparison: 2 Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy rate, outcome: 2.1 clinical pregnancy rate per couple

Comparison 1: Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer, Outcome 1: Live birth per couple

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Analysis 1.1

Comparison 1: Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer, Outcome 1: Live birth per couple

Comparison 1: Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer, Outcome 2: Live birth per couple: grouped by number of embryos transferred

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Analysis 1.2

Comparison 1: Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer, Outcome 2: Live birth per couple: grouped by number of embryos transferred

Comparison 1: Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer, Outcome 3: Live birth rate per couple: grouped by prognosis

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Analysis 1.3

Comparison 1: Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer, Outcome 3: Live birth rate per couple: grouped by prognosis

Comparison 1: Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer, Outcome 4: Live birth rate: grouped by day of randomisation

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Analysis 1.4

Comparison 1: Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer, Outcome 4: Live birth rate: grouped by day of randomisation

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 1: Cumulative pregnancy rate from fresh and frozen transfers

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Analysis 2.1

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 1: Cumulative pregnancy rate from fresh and frozen transfers

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 2: Cumulative pregnancy rate per couple: grouped by number of embryos transferred

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Analysis 2.2

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 2: Cumulative pregnancy rate per couple: grouped by number of embryos transferred

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 3: Cumulative pregnancy rate per couple: grouped by prognosis

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Analysis 2.3

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 3: Cumulative pregnancy rate per couple: grouped by prognosis

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 4: Cumulative pregnancy rate: grouped by day of randomisation

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Analysis 2.4

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 4: Cumulative pregnancy rate: grouped by day of randomisation

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 5: Cumulative pregnancy rate from fresh and frozen transfers: grouped by vitrification or slow freezing

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Analysis 2.5

Comparison 2: Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer, Outcome 5: Cumulative pregnancy rate from fresh and frozen transfers: grouped by vitrification or slow freezing

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 1: Clinical pregnancy rate per couple

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Analysis 3.1

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 1: Clinical pregnancy rate per couple

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 2: Clinical pregnancy rate per couple: grouped by number of embryos transferred

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Analysis 3.2

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 2: Clinical pregnancy rate per couple: grouped by number of embryos transferred

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 3: Clinical pregnancy rate per couple: grouped by prognosis

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Analysis 3.3

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 3: Clinical pregnancy rate per couple: grouped by prognosis

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 4: Clinical pregnancy rate per couple: grouped by day of randomisation

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Analysis 3.4

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 4: Clinical pregnancy rate per couple: grouped by day of randomisation

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 5: Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage

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Analysis 3.5

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 5: Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 6: Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus TLS (with algorithm) blastocyst stage

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Analysis 3.6

Comparison 3: Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer, Outcome 6: Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus TLS (with algorithm) blastocyst stage

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 1: Multiple pregnancy rate per couple

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Analysis 4.1

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 1: Multiple pregnancy rate per couple

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 2: Multiple pregnancy rate per couple: grouped by number of embryos transferred

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Analysis 4.2

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 2: Multiple pregnancy rate per couple: grouped by number of embryos transferred

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 3: Multiple pregnancy rate per couple: grouped by prognosis

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Analysis 4.3

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 3: Multiple pregnancy rate per couple: grouped by prognosis

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 4: Multiple pregnancy rate per couple: grouped by day of randomisation

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Analysis 4.4

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 4: Multiple pregnancy rate per couple: grouped by day of randomisation

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 5: High‐order pregnancies (more than 2 gestational sacs) per couple

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Analysis 4.5

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 5: High‐order pregnancies (more than 2 gestational sacs) per couple

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 6: Multiple pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage

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Analysis 4.6

Comparison 4: Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer, Outcome 6: Multiple pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage

Comparison 5: Blastocyst‐ versus cleavage‐stage transfer: miscarriage rate following fresh transfer, Outcome 1: Miscarriage rate per couple

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Analysis 5.1

Comparison 5: Blastocyst‐ versus cleavage‐stage transfer: miscarriage rate following fresh transfer, Outcome 1: Miscarriage rate per couple

Comparison 6: Blastocyst‐ versus cleavage‐stage transfer: embryo freezing rate per couple, Outcome 1: Embryo freezing per couple

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Analysis 6.1

Comparison 6: Blastocyst‐ versus cleavage‐stage transfer: embryo freezing rate per couple, Outcome 1: Embryo freezing per couple

Comparison 7: Blastocyst‐ versus cleavage‐stage transfer: failure rate to transfer embryos (per couple), Outcome 1: Failure to transfer any embryos (per couple)

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Analysis 7.1

Comparison 7: Blastocyst‐ versus cleavage‐stage transfer: failure rate to transfer embryos (per couple), Outcome 1: Failure to transfer any embryos (per couple)

Summary of findings 1. Blastocyst‐stage versus cleavage‐stage embryo transfer for assisted reproductive technology

Blastocyst‐stage versus cleavage‐stage embryo transfer for assisted reproductive technology

Population: women and couples with subfertility
Settings: assisted reproductive technology
Intervention: blastocyst‐stage embryo transfer
Comparison: cleavage‐stage embryo transfer

Outcomes per couple

Illustrative comparative risks* (95% CI)

Relative effect
(95% CI)

No. of participants
(studies)

Quality of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Cleavage‐stage embryo transfer

Blastocyst‐stage embryo transfer

Live birth rate per fresh transfer

312 per 1000

365 per 1000

(324 to 406)

OR 1.27
(1.06 to 1.51)

2219

(15 studies)

⊕⊕⊝⊝
Lowa,c

When sensitivity analysis restricted to 9 studies with low or some concerns of overall risk of bias, it results in a similar effect (OR 1.26, 95% CI 1.04 to 1.54).

Cumulative pregnancy rate (slow freezing)

565 per 1000

472 per 1000

(384 to 562)

OR 0.69

(0.48 to 0.99)

512

(4 studies)

⊕⊕⊝⊝
Lowa,c

Cumulative pregnancy rate (vitrification)

333 per 1000

550 per 1000

(369 to 719)

OR 2.44

(1.17 to 5.12)

120

(1 study)

⊕⊕⊕⊝ Moderatea

Clinical pregnancy rate

390 per 1000

444 per 1000
(417 to 470)

OR 1.25
(1.12 to 1.39)

5821
(32 studies)

⊕⊕⊝⊝
Moderatea

When sensitivity analysis restricted to 17 studies with low risk or some concerns of overall risk of bias, it results in a similar effect (OR 1.24, 95% CI 1.08 to 1.41).

Multiple pregnancy rate

89 per 1000

99 per 1000
(81 to 119)

OR 1.12
(0.90 to 1.38)

4208
(22 studies)

⊕⊕⊝⊝
Lowa,b,c

When sensitivity analysis restricted to 15 studies with low risk or some concerns of overall risk of bias, it results in an increase of multiple pregnancy rate (OR 1.33, 95% CI 1.04 to 1.70).

Miscarriage rate

67 per 1000

82 per 1000
(68 to 111)

OR 1.24, (0.98 to 1.57)

4106
(21 studies)

⊕⊕⊝⊝
Lowa,c

Embryo freezing rate

594 per 1000

412 per 1000

(369 to 455)

OR 0.48

(0.40 to 0.57)

2292

(14 studies)

⊕⊕⊝⊝
Lowa,b

I2 = 84%. Direction of effect largely consistent

Failure rate to transfer any embryos

11 per 1000

26 per 1000

(19 to 37)

OR 2.50

(1.76 to 3.55)

2577

(17 studies)

⊕⊕⊕⊝
Moderatea

I2 = 36%

*The basis for the assumed risk is the median control group risk across studies. The corresponding risk (and its 95% confidence interval) is based on the assumed risk in the comparison group and the relative effect of the intervention (and its 95% CI).
CI: confidence interval; OR: odds ratio

GRADE Working Group grades of evidence
High quality: further research is very unlikely to change our confidence in the estimate of effect.
Moderate quality: further research is likely to have an important impact on our confidence in the estimate of effect and may change the estimate.
Low quality: further research is very likely to have an important impact on our confidence in the estimate of effect and is likely to change the estimate.
Very low quality: we are very uncertain about the estimate.

aDowngraded one level for serious risk of bias: most studies have some concerns of overall risk of bias, mainly due to the randomisation process, deviations from the intended intervention and selective reporting
bDowngraded one level for serious inconsistency
cDowngraded one level for serious imprecision: findings compatible with benefit or minimal effect

Figuras y tablas -
Summary of findings 1. Blastocyst‐stage versus cleavage‐stage embryo transfer for assisted reproductive technology
Table 1. Culture techniques of included studies

Trial

Culture technique day 2/3

Culture technique day 5/6

Aziminekoo 2015

Sydney IVF cleavage medium, Cook

Sydney IVF blastocyst medium

Brugnon 2010

G series™ medium (Vitrolife, Sweden)

G series™ medium (Vitrolife, Sweden)

Bungum 2003

Sequential G1 Vitrolife

Sequential G1/G2 Vitrolife

Coskun 2000

Sequential MediCult

Sequential G1/G2 Vitrolife

Devreker 2000

NS

NS

Elgindy 2011

NS

NS

Emiliani 2003

In‐house sequential (based on G1/G2)

In‐house sequential (based on G1/G2)

Fernandez‐Shaw 2015

Sequential G1 Vitrolife

Sequential G1/G2 Vitrolife

Fisch 2007

NS

NS

Frattarelli 2003

NS

NS

Gaafar 2015

NS

NS

Gardner 1998a

Single Ham's F10 In‐house

Sequential G1/G2 In‐house

Hatirnaz 2017

Standard culture medium

Sequential G1/G2 Scandinavian IVF Sciences

Hreinsson 2004

Vitrolife IVF

Sequential G1/G2 or CCM Vitrolife

Karaki 2002

MediCult

Sequential G1/G2 Vitrolife

Kaser 2017

Global total with HSA LifeGlobal

Global total with HSA LifeGlobal

Kaur 2014

Cleavage medium

G2 Plus media

Kolibianakis 2004

Sequential G1 Vitrolife

Sequential G1/G2 Vitrolife

Levi‐Setti 2018

NS

NS

Levitas 2004

NS

Sequential ‐ G1/G2 Vitrolife

Levron 2002

NS

NS

Livingstone 2002

Sequential ‐ Sydney IVF Cook

Sequential ‐ Sydney IVF Cook

Motta 1998

Sequential ‐ Irvines P1

Sequential ‐ Irvines P1 then Blast media

Pantos 2004

Papanikolaou 2005

Sequential ‐ Vitrolife G1/G2 GII or GIII

Sequential ‐ Vitrolife G1/G2 GII or GIII

Papanikolaou 2006

Assume sequential ‐ Vitrolife G1/G2

Assume sequential ‐ Vitrolife G1/G2

Rienzi 2002

Sequential G1 Vitrolife

Sequential G1/G2 Vitrolife

Schillaci 2002

NS

NS

Singh 2017

NS

NS

Ten 2011

NS

NS

Van der Auwera 2002

Sequential both Cook and Vitrolife

Sequential both Cook and Vitrolife

Yang 2018

Sequential media (G1.5, Vitrolife) in a Primo Vision time‐lapse system (Vitrolife)

Sequential G1/G2 Vitrolife

CCM: a Vitrolife trademarked medium for blastocyst culture
IVF: in vitro fertilisation
G1/G2:sequential media from Vitrolife
NS: not stated

Figuras y tablas -
Table 1. Culture techniques of included studies
Table 2. Blastocyst formation and implantation rate (in day 5 to 6 transfers)

Study

Blastocyst formation rate

Implantation D2/3

Implantation D5/6

Other

Aziminekoo 2015

22.4%

21/173; 12.1%

22/152; 14.5%

Brugnon 2010

Not stated

24/52; 46.2%

23/55; 41.8%

Bungum 2003

55.2%

50/114; 43.9%

44/120; 36.7%

2/61 participants had only 1 blastocyst

Coskun 2000

28%

50/235; 21.3%

52/218; 23.9%

77% participants had at least 1 blastocyst

Devreker 2000

Not stated

1/34; 2.9%

8/19; 42.1%

Elgindy 2011

97%

71/197; 36%

53/280; 19%

Emiliani 2003

48%

57/197; 28.9%

50/168; 29.8%

Fernandez‐Shaw 2015

67.7 %

20/71; 28.1%

36/84; 42.8%

Fisch 2007

Not stated

11/12; 92%

4/8; 50%

Frattarelli 2003

Not stated

18/69; 26.1%

23/53; 43.4%

Gaafar 2015

Not stated

Not stated

Not stated

Gardner 1998a

46.5%

64/174; 36.8%

53/95; 55.8%

85% women had at least 2 blastocysts

Hatirnaz 2017

52.6%

45/95; 47.4%

43/95; 45.3%

Hreinsson 2004

33%

29/139; 20.9%

24/114; 21.1%

2 morula replaced (one implanted). 60% pregnancy rate when top‐quality blasts transferred

Karaki 2002

33%

37/291 12.7%

37/142; 26.1%

9/80 cancelled due to lack of blastocysts (unselected)

Kaser 2017

Not stated

23/56; 41.1%

26/53; 49.1%

Kaur 2014

Not stated

66/309; 21.4%

102/290; 35.2%

Kolibianakis 2004

50.7%

96/234; 41.0%

94/226; 41.6%

Levi‐Setti 2018

Not stated

25.67%

28.37%

Levitas 2004

43%

4/56; 7.1%

10/24; 4.2%

Day 5‐7 26% cancelled due to lack of blastocysts (poor prognosis)

Levron 2002

34.2%

53/137; 38.7%

20/99; 20.2%

6.5% cancelled due to lack of blastocysts (good prognosis)

Livingstone 2002

Not stated

Motta 1998

Not stated

51/262; 19.5%

36/120; 30.0%

6/58 cycles cancelled D5 no blastocysts

Pantos 2004

44.6%

15.8%

15.8%

Papanikolaou 2005

Not stated

35/170; 20.6%

59/158; 37.3%

4/158 women had only 1 blast transferred due to lack of availability and 1 had it on request

Papanikolaou 2006

Not stated

38/156; 24%

58/149; 38.9%

Number of participants with no embryos available D3: 8 and D5: 11

Rienzi 2002

44.8%

34/96; 35.4%

38/100; 38.0%

Good prognosis

Schillaci 2002

60.3%

23/168; 13.7%

26/110; 23.6%

Unselected population nil cancellations D5

Singh 2017

Not stated

Not stated

Not stated

Ten 2011

Not stated

21/54; 38.9%

26/56; 46.4%

Good prognosis

Van der Auwera 2002

44.7%

31/106; 29.2%

41/90; 45.6%

27% cancellation D5 (unselected population)

Yang 2018

Not stated

80/290; 62.1%

22/306; 72.5%

Figuras y tablas -
Table 2. Blastocyst formation and implantation rate (in day 5 to 6 transfers)
Table 3. Mean number of embryos transferred

Study ID

Day 2/3

Day 5/6

Aziminekoo 2015

2.8 ± 1.1

2.6 ± 0.6

Brugnon 2010

1.0 ± 0

1.0 ± 0

Bungum 2003

2.0 ± NS

2.0 ± NS

Coskun 2000

2.3 ± 0.6

2.2 ± 0.5

Devreker 2000

2.8 ± NS

1.7 ± NS

Elgindy 2011

2.8 ± 0.4

2.0 ± 0.2

Emiliani 2003

2.1 ± 0.4

1.9 ± 0.3

Fernandez‐Shaw 2015

1.5 ± 0.5

1.4 ± 0.5

Fisch 2007

1.0 ± 0

1.0 ± 0

Frattarelli 2003

3.0 ± 0.5

2.0 ± 0.2

Gaafar 2015

NS

NS

Gardner 1998a

3.7 ± 0.1

2.2 ± 0.1

Hatirnaz 2017

1.4 ± 0.6

1.4 ± 0.4

Hreinsson 2004

1.8 ± NS

1.9 ± NS

Karaki 2002

3.5 ± 0.6

2.0 ± 0.1

Kaser 2017

1.0 ± 0

1.0 ± 0

Kaur 2014

2.0 ± 0.7

1.9 ± 0.5

Kolibianakis 2004

1.9 ± 0.1

1.8 ± 0.1

Levi‐Setti 2018

1.9 ± 0.4

1.8 ± 0.6

Levitas 2004

3.4 ± NS

1.9 ± NS

Levron 2002

3.1 ± 0.6

2.3 ± 0.8

Livingstone 2002

2.0 ± NS

1.0 ± NS

Motta 1998

4.6 ± NS

2.3 ± NS

Pantos 2004

4.0 ± 1.5

3.4 ± 1.1

Papanikolaou 2005

2.0 ± 0

2.0 ± 0.5

Papanikolaou 2006

1.0 ± 0

1.0 ± 0

Rienzi 2002

2.0 ± 0

2.0 ± 0

Schillaci 2002

2.8

1.8

Singh 2017

NS

NS

Ten 2011

2.0 ± NS

2.0 ± NS

Van der Auwera 2002

1.9 ± 0.3

1.9 ± 0.2

Yang 2018

1.0 ± 0

1.0 ± 0

NS ‐ not stated

Figuras y tablas -
Table 3. Mean number of embryos transferred
Comparison 1. Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

1.1 Live birth per couple Show forest plot

15

2219

Odds Ratio (M‐H, Fixed, 95% CI)

1.27 [1.06, 1.51]

1.2 Live birth per couple: grouped by number of embryos transferred Show forest plot

15

2677

Odds Ratio (M‐H, Fixed, 95% CI)

1.30 [1.10, 1.53]

1.2.1 More cleavage‐stage than blastocyst embryos transferred

6

483

Odds Ratio (M‐H, Fixed, 95% CI)

1.51 [1.03, 2.22]

1.2.2 Single embryo transfer

2

458

Odds Ratio (M‐H, Fixed, 95% CI)

1.47 [0.98, 2.20]

1.2.3 Equal number of embryos transferred

9

1736

Odds Ratio (M‐H, Fixed, 95% CI)

1.21 [0.99, 1.47]

1.3 Live birth rate per couple: grouped by prognosis Show forest plot

15

Odds Ratio (M‐H, Fixed, 95% CI)

Subtotals only

1.3.1 good prognostic factors

9

1514

Odds Ratio (M‐H, Fixed, 95% CI)

1.28 [1.04, 1.59]

1.3.2 poor prognostic factors

2

77

Odds Ratio (M‐H, Fixed, 95% CI)

2.05 [0.53, 7.96]

1.3.3 unselected group

4

628

Odds Ratio (M‐H, Fixed, 95% CI)

1.19 [0.86, 1.66]

1.4 Live birth rate: grouped by day of randomisation Show forest plot

15

Odds Ratio (M‐H, Fixed, 95% CI)

Subtotals only

1.4.1 randomisation at start of cycle

6

1207

Odds Ratio (M‐H, Fixed, 95% CI)

1.08 [0.84, 1.38]

1.4.2 randomised on day of OPU and day 1 after OPU

5

566

Odds Ratio (M‐H, Fixed, 95% CI)

1.16 [0.82, 1.65]

1.4.3 randomised day 2 to 3 post‐OPU

2

364

Odds Ratio (M‐H, Fixed, 95% CI)

2.17 [1.42, 3.33]

1.4.4 day of randomisation unstated

2

82

Odds Ratio (M‐H, Fixed, 95% CI)

1.71 [0.67, 4.39]

Figuras y tablas -
Comparison 1. Blastocyst‐ versus cleavage‐stage transfer: live birth rate following fresh transfer
Comparison 2. Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

2.1 Cumulative pregnancy rate from fresh and frozen transfers Show forest plot

5

632

Odds Ratio (M‐H, Fixed, 95% CI)

0.89 [0.64, 1.22]

2.2 Cumulative pregnancy rate per couple: grouped by number of embryos transferred Show forest plot

5

739

Odds Ratio (M‐H, Fixed, 95% CI)

0.88 [0.65, 1.18]

2.2.1 single embryo transfer

1

107

Odds Ratio (M‐H, Fixed, 95% CI)

0.84 [0.39, 1.79]

2.2.2 equal number of embryos transferred

5

632

Odds Ratio (M‐H, Fixed, 95% CI)

0.89 [0.64, 1.22]

2.3 Cumulative pregnancy rate per couple: grouped by prognosis Show forest plot

5

632

Odds Ratio (M‐H, Fixed, 95% CI)

0.89 [0.64, 1.22]

2.3.1 good prognostic factors

2

205

Odds Ratio (M‐H, Fixed, 95% CI)

0.54 [0.30, 0.98]

2.3.2 unselected group

3

427

Odds Ratio (M‐H, Fixed, 95% CI)

1.10 [0.74, 1.61]

2.4 Cumulative pregnancy rate: grouped by day of randomisation Show forest plot

5

632

Odds Ratio (M‐H, Fixed, 95% CI)

0.89 [0.64, 1.22]

2.4.1 randomisation at start of cycle

3

414

Odds Ratio (M‐H, Fixed, 95% CI)

0.81 [0.54, 1.20]

2.4.2 randomised on day of OPU and day 1 after OPU

2

218

Odds Ratio (M‐H, Fixed, 95% CI)

1.06 [0.61, 1.83]

2.5 Cumulative pregnancy rate from fresh and frozen transfers: grouped by vitrification or slow freezing Show forest plot

5

Odds Ratio (M‐H, Fixed, 95% CI)

Subtotals only

2.5.1 slow freezing

4

512

Odds Ratio (M‐H, Fixed, 95% CI)

0.69 [0.48, 0.99]

2.5.2 vitrification

1

120

Odds Ratio (M‐H, Fixed, 95% CI)

2.44 [1.17, 5.12]

Figuras y tablas -
Comparison 2. Blastocyst‐ versus cleavage‐stage transfer: cumulative pregnancy rate following fresh and frozen transfer
Comparison 3. Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

3.1 Clinical pregnancy rate per couple Show forest plot

32

5821

Odds Ratio (M‐H, Fixed, 95% CI)

1.25 [1.12, 1.39]

3.2 Clinical pregnancy rate per couple: grouped by number of embryos transferred Show forest plot

32

7062

Odds Ratio (M‐H, Fixed, 95% CI)

1.26 [1.14, 1.38]

3.2.1 equal number of embryo transfers

20

4434

Odds Ratio (M‐H, Fixed, 95% CI)

1.31 [1.16, 1.48]

3.2.2 more cleavage stage than blastocyst embryos transferred

12

1387

Odds Ratio (M‐H, Fixed, 95% CI)

1.07 [0.86, 1.33]

3.2.3 single embryo transfer

5

1241

Odds Ratio (M‐H, Fixed, 95% CI)

1.31 [1.04, 1.65]

3.3 Clinical pregnancy rate per couple: grouped by prognosis Show forest plot

32

5821

Odds Ratio (M‐H, Fixed, 95% CI)

1.25 [1.12, 1.39]

3.3.1 good prognostic factors

19

3645

Odds Ratio (M‐H, Fixed, 95% CI)

1.25 [1.09, 1.43]

3.3.2 poor prognostic factors

3

195

Odds Ratio (M‐H, Fixed, 95% CI)

1.62 [0.84, 3.10]

3.3.3 unselected group

10

1981

Odds Ratio (M‐H, Fixed, 95% CI)

1.22 [1.01, 1.46]

3.4 Clinical pregnancy rate per couple: grouped by day of randomisation Show forest plot

32

5821

Odds Ratio (M‐H, Fixed, 95% CI)

1.25 [1.12, 1.39]

3.4.1 randomised start of cycle

8

1759

Odds Ratio (M‐H, Fixed, 95% CI)

1.12 [0.92, 1.37]

3.4.2 randomised on day of OPU or day 1

13

2094

Odds Ratio (M‐H, Fixed, 95% CI)

1.19 [1.00, 1.42]

3.4.3 randomised on day 2 to 3

6

1275

Odds Ratio (M‐H, Fixed, 95% CI)

1.50 [1.19, 1.88]

3.4.4 day of randomisation unstated

5

693

Odds Ratio (M‐H, Fixed, 95% CI)

1.33 [0.98, 1.80]

3.5 Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage Show forest plot

2

709

Odds Ratio (M‐H, Fixed, 95% CI)

1.41 [1.04, 1.90]

3.6 Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus TLS (with algorithm) blastocyst stage Show forest plot

1

110

Odds Ratio (M‐H, Fixed, 95% CI)

0.91 [0.43, 1.96]

Figuras y tablas -
Comparison 3. Blastocyst‐ versus cleavage‐stage transfer: clinical pregnancy following fresh transfer
Comparison 4. Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

4.1 Multiple pregnancy rate per couple Show forest plot

22

4208

Odds Ratio (M‐H, Fixed, 95% CI)

1.12 [0.90, 1.38]

4.2 Multiple pregnancy rate per couple: grouped by number of embryos transferred Show forest plot

22

5159

Odds Ratio (M‐H, Fixed, 95% CI)

1.12 [0.91, 1.38]

4.2.1 equal number of embryos transferred

14

3399

Odds Ratio (M‐H, Fixed, 95% CI)

1.29 [1.01, 1.65]

4.2.2 more cleavage stage than blastocyst embryos transferred

8

809

Odds Ratio (M‐H, Fixed, 95% CI)

0.75 [0.49, 1.13]

4.2.3 single embryo transfer

2

951

Odds Ratio (M‐H, Fixed, 95% CI)

1.22 [0.51, 2.91]

4.3 Multiple pregnancy rate per couple: grouped by prognosis Show forest plot

22

4208

Odds Ratio (M‐H, Fixed, 95% CI)

1.12 [0.90, 1.38]

4.3.1 good prognostic factors

15

2904

Odds Ratio (M‐H, Fixed, 95% CI)

1.14 [0.89, 1.46]

4.3.2 poor prognostic factors

1

54

Odds Ratio (M‐H, Fixed, 95% CI)

0.89 [0.14, 5.81]

4.3.3 unselected

6

1250

Odds Ratio (M‐H, Fixed, 95% CI)

1.07 [0.71, 1.59]

4.4 Multiple pregnancy rate per couple: grouped by day of randomisation Show forest plot

22

4208

Odds Ratio (M‐H, Fixed, 95% CI)

1.12 [0.90, 1.38]

4.4.1 randomised start of cycle

7

1704

Odds Ratio (M‐H, Fixed, 95% CI)

1.02 [0.71, 1.46]

4.4.2 randomised on day of OPU or day 1

9

1647

Odds Ratio (M‐H, Fixed, 95% CI)

1.05 [0.73, 1.52]

4.4.3 randomised on day 2 to 3

4

682

Odds Ratio (M‐H, Fixed, 95% CI)

1.71 [1.14, 2.56]

4.4.4 day of randomisation unstated

2

175

Odds Ratio (M‐H, Fixed, 95% CI)

0.21 [0.06, 0.70]

4.5 High‐order pregnancies (more than 2 gestational sacs) per couple Show forest plot

13

2335

Odds Ratio (M‐H, Fixed, 95% CI)

0.45 [0.18, 1.15]

4.6 Multiple pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage Show forest plot

1

600

Odds Ratio (M‐H, Fixed, 95% CI)

1.59 [0.61, 4.17]

Figuras y tablas -
Comparison 4. Blastocyst‐ versus cleavage‐stage transfer: multiple pregnancy following fresh transfer
Comparison 5. Blastocyst‐ versus cleavage‐stage transfer: miscarriage rate following fresh transfer

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

5.1 Miscarriage rate per couple Show forest plot

21

4106

Odds Ratio (M‐H, Fixed, 95% CI)

1.24 [0.98, 1.57]

Figuras y tablas -
Comparison 5. Blastocyst‐ versus cleavage‐stage transfer: miscarriage rate following fresh transfer
Comparison 6. Blastocyst‐ versus cleavage‐stage transfer: embryo freezing rate per couple

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

6.1 Embryo freezing per couple Show forest plot

14

2292

Odds Ratio (M‐H, Fixed, 95% CI)

0.48 [0.40, 0.57]

Figuras y tablas -
Comparison 6. Blastocyst‐ versus cleavage‐stage transfer: embryo freezing rate per couple
Comparison 7. Blastocyst‐ versus cleavage‐stage transfer: failure rate to transfer embryos (per couple)

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

7.1 Failure to transfer any embryos (per couple) Show forest plot

17

2577

Odds Ratio (M‐H, Fixed, 95% CI)

2.50 [1.76, 3.55]

Figuras y tablas -
Comparison 7. Blastocyst‐ versus cleavage‐stage transfer: failure rate to transfer embryos (per couple)
Risk of bias for analysis 1.1 Live birth per couple

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All randomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methods are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalised before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 1.1 Live birth per couple
Risk of bias for analysis 1.2 Live birth per couple: grouped by number of embryos transferred

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 1.2.1 More cleavage‐stage than blastocyst embryos transferred

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All randomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Subgroup 1.2.2 Single embryo transfer

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Subgroup 1.2.3 Equal number of embryos transferred

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methods are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalised before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 1.2 Live birth per couple: grouped by number of embryos transferred
Risk of bias for analysis 1.3 Live birth rate per couple: grouped by prognosis

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 1.3.1 good prognostic factors

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All randomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalised before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Subgroup 1.3.2 poor prognostic factors

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Subgroup 1.3.3 unselected group

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methods are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 1.3 Live birth rate per couple: grouped by prognosis
Risk of bias for analysis 1.4 Live birth rate: grouped by day of randomisation

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 1.4.1 randomisation at start of cycle

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methods are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalised before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Subgroup 1.4.2 randomised on day of OPU and day 1 after OPU

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Subgroup 1.4.3 randomised day 2 to 3 post‐OPU

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All randomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Subgroup 1.4.4 day of randomisation unstated

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Figuras y tablas -
Risk of bias for analysis 1.4 Live birth rate: grouped by day of randomisation
Risk of bias for analysis 2.1 Cumulative pregnancy rate from fresh and frozen transfers

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

information. Only proportions were reproted

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 2.1 Cumulative pregnancy rate from fresh and frozen transfers
Risk of bias for analysis 2.2 Cumulative pregnancy rate per couple: grouped by number of embryos transferred

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 2.2.1 single embryo transfer

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

information. Only proportions were reproted

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Subgroup 2.2.2 equal number of embryos transferred

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

information. Only proportions were reproted

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 2.2 Cumulative pregnancy rate per couple: grouped by number of embryos transferred
Risk of bias for analysis 2.3 Cumulative pregnancy rate per couple: grouped by prognosis

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 2.3.1 good prognostic factors

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

No information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Subgroup 2.3.2 unselected group

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 2.3 Cumulative pregnancy rate per couple: grouped by prognosis
Risk of bias for analysis 2.4 Cumulative pregnancy rate: grouped by day of randomisation

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 2.4.1 randomisation at start of cycle

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

No information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methods are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Subgroup 2.4.2 randomised on day of OPU and day 1 after OPU

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 2.4 Cumulative pregnancy rate: grouped by day of randomisation
Risk of bias for analysis 2.5 Cumulative pregnancy rate from fresh and frozen transfers: grouped by vitrification or slow freezing

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 2.5.1 slow freezing

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

No information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Subgroup 2.5.2 vitrification

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 2.5 Cumulative pregnancy rate from fresh and frozen transfers: grouped by vitrification or slow freezing
Risk of bias for analysis 3.1 Clinical pregnancy rate per couple

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Low risk of bias High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

No information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

High risk due to deviation from the intended interventions and bias due to missing outcome data

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. All 118 randomised women were analysed.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias High risk of bias High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to the randomisation process, deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All ranomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. All women randomised were analysed

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fisch 2007

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Although the number of missing outcomes is high, there is no evidence of bias about it

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is some risk of bias due to the randomisation process, to deviations from the intended interventions and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Gaafar 2015

Low risk of bias Some concerns High risk of bias Low risk of bias Some concerns High risk of bias

Quote "Randomization was done by computer permuted blocks size of 4, allocation by closed envelops, parallel technique" No mention about opaque envelopes

Not evidence of potential of concerns generating a substantial impact

A large proportion of missing outcomes: 326 were eligible. 126 cases had day 2/3 transfer and 126 had blastocyst transfer.

Clinical pregnancy with cardiac pulsation four weeks after ET. PACTR201308000581376 Quote "Masking Care giver/Provider,Outcome assessors,Participants"

There is only a difference in outcome reporting regarding multiple pregnancies

High bias due to missing outcome data and some concerns due to deviations from intended interventions and bias in selection of the reported result

Gardner 1998a

Some concerns High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

Concealment was not reported, there was a difference in Previous no. of cycles

No effort for blindness is described. There was a difference No. of embryos transferred and proportion of embryo freezing that likely have affected the outcome

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

ClinicalTrials.gov Identifier: NCT03764865

High risk of bias due to deviations from intended intervention

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignment

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations of the protocol and some concerns of risk of bias due to selection of reported results.

Kaser 2017

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

The observed number of events is much greater than the number of participants with missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote:"NCT02218255"

There are some concerns of risk of bias due to deviations from the intended interventions.

Kaur 2014

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to the randomisation process and deviations from the intended interventions, and some concerns of risk of bias due to selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalized before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Pantos 2004

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

There is no information about the method of measuring the outcome, but it is probable that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Schillaci 2002

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Singh 2017

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealment and no information about the baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

It is not possible to know if there were missing outcome data.

Method of measuring the outcome was not informed, but it was probably not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is a high risk of bias due to deviations from the intended interventions and missing outcomes data. And some concerns of risk of bias due to randomisation process and selection of reported results.

Ten 2011

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the analysis that was performed.

No information about neither the absolute number of events nor the missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to the randomisation process, deviations from the intended interventions and missing outcomes, and some concerns of risk of bias due to randomisation process and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Figuras y tablas -
Risk of bias for analysis 3.1 Clinical pregnancy rate per couple
Risk of bias for analysis 3.2 Clinical pregnancy rate per couple: grouped by number of embryos transferred

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 3.2.1 equal number of embryo transfers

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Low risk of bias High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

No information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

High risk due to deviation from the intended interventions and bias due to missing outcome data

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. All 118 randomised women were analysed.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. All women randomised were analysed

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fisch 2007

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Although the number of missing outcomes is high, there is no evidence of bias about it

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to the randomisation process, due to deviations from the intended interventions and selection of reported results.

Gaafar 2015

Low risk of bias Some concerns High risk of bias Low risk of bias Some concerns Some concerns

Quote "Randomization was done by computer permuted blocks size of 4, allocation by closed envelops, parallel technique" No mention about opaque envelopes

Not evidence of potential of concerns generating a substantial impact

A large proportion of missing outcomes: 326 were eligible. 126 cases had day 2/3 transfer and 126 had blastocyst transfer.

Clinical pregnancy with cardiac pulsation four weeks after ET. PACTR201308000581376 Quote "Masking Care giver/Provider,Outcome assessors,Participants"

There is only a difference in outcome reporting regarding multiple pregnancies

High bias due to missing outcome data and some concerns due to deviations from intended interventions and bias in selection of the reported result

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignment

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Kaser 2017

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

The observed number of events is much greater than the number of participants with missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote:"NCT02218255"

There are some concerns of risk of bias due to deviations from the intended interventions.

Kaur 2014

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to the randomisation process and deviations from the intended interventions, and some concerns of risk of bias due to selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalized before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Singh 2017

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealment and no information about the baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

It is not possible to know if there were missing outcome data.

Method of measuring the outcome was not informed, but it was probably not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is a high risk of bias due to deviations from the intended interventions and missing outcomes data. And some concerns of risk of bias due to randomisation process and selection of reported results.

Ten 2011

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the analysis that was performed.

No information about neither the absolute number of events nor the missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and missing outcomes, and some concerns of risk of bias due to randomisation process and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Subgroup 3.2.2 more cleavage stage than blastocyst embryos transferred

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All ranomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Gardner 1998a

Some concerns High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

Concealment was not reported, there was a difference in Previous no. of cycles

No effort for blindness is described. There was a difference No. of embryos transferred and proportion of embryo freezing that likely have affected the outcome

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

ClinicalTrials.gov Identifier: NCT03764865

High risk of bias due to deviations from intended intervention

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations of the protocol and some concerns of risk of bias due to selection of reported results.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Pantos 2004

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

There is no information about the method of measuring the outcome, but it is probable that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Schillaci 2002

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Subgroup 3.2.3 single embryo transfer

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Low risk of bias High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

No information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

High risk due to deviation from the intended interventions and bias due to missing outcome data

Fisch 2007

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Although the number of missing outcomes is high, there is no evidence of bias about it

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to the randomisation process, due to deviations from the intended interventions and selection of reported results.

Kaser 2017

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

The observed number of events is much greater than the number of participants with missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote:"NCT02218255"

There are some concerns of risk of bias due to deviations from the intended interventions.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Figuras y tablas -
Risk of bias for analysis 3.2 Clinical pregnancy rate per couple: grouped by number of embryos transferred
Risk of bias for analysis 3.3 Clinical pregnancy rate per couple: grouped by prognosis

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 3.3.1 good prognostic factors

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Low risk of bias High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

No information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

High risk due to deviation from the intended interventions and bias due to missing outcome data

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. All 118 randomised women were analysed.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All ranomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Fisch 2007

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Although the number of missing outcomes is high, there is no evidence of bias about it

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to the randomisation process, due to deviations from the intended interventions and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Gardner 1998a

Some concerns High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

Concealment was not reported, there was a difference in Previous no. of cycles

No effort for blindness is described. There was a difference No. of embryos transferred and proportion of embryo freezing that likely have affected the outcome

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

ClinicalTrials.gov Identifier: NCT03764865

High risk of bias due to deviations from intended intervention

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignment

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Kaser 2017

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

The observed number of events is much greater than the number of participants with missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote:"NCT02218255"

There are some concerns of risk of bias due to deviations from the intended interventions.

Kaur 2014

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalized before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Singh 2017

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealment and no information about the baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

It is not possible to know if there were missing outcome data.

Method of measuring the outcome was not informed, but it was probably not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is a high risk of bias due to deviations from the intended interventions and missing outcomes data. And some concerns of risk of bias due to randomisation process and selection of reported results.

Ten 2011

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the analysis that was performed.

No information about neither the absolute number of events nor the missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and missing outcomes, and some concerns of risk of bias due to randomisation process and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Subgroup 3.3.2 poor prognostic factors

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Subgroup 3.3.3 unselected group

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. All women randomised were analysed

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Gaafar 2015

Low risk of bias Some concerns High risk of bias Low risk of bias Some concerns Some concerns

Quote "Randomization was done by computer permuted blocks size of 4, allocation by closed envelops, parallel technique" No mention about opaque envelopes

Not evidence of potential of concerns generating a substantial impact

A large proportion of missing outcomes: 326 were eligible. 126 cases had day 2/3 transfer and 126 had blastocyst transfer.

Clinical pregnancy with cardiac pulsation four weeks after ET. PACTR201308000581376 Quote "Masking Care giver/Provider,Outcome assessors,Participants"

There is only a difference in outcome reporting regarding multiple pregnancies

High bias due to missing outcome data and some concerns due to deviations from intended interventions and bias in selection of the reported result

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations of the protocol and some concerns of risk of bias due to selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to the randomisation process and deviations from the intended interventions, and some concerns of risk of bias due to selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Pantos 2004

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

There is no information about the method of measuring the outcome, but it is probable that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Schillaci 2002

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 3.3 Clinical pregnancy rate per couple: grouped by prognosis
Risk of bias for analysis 3.4 Clinical pregnancy rate per couple: grouped by day of randomisation

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 3.4.1 randomised start of cycle

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Low risk of bias High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

No information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

High risk due to deviation from the intended interventions and bias due to missing outcome data

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Gardner 1998a

Some concerns High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

Concealment was not reported, there was a difference in Previous no. of cycles

No effort for blindness is described. There was a difference No. of embryos transferred and proportion of embryo freezing that likely have affected the outcome

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

ClinicalTrials.gov Identifier: NCT03764865

High risk of bias due to deviations from intended intervention

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to the randomisation process and deviations from the intended interventions, and some concerns of risk of bias due to selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalized before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Subgroup 3.4.2 randomised on day of OPU or day 1

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. All women randomised were analysed

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fisch 2007

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Although the number of missing outcomes is high, there is no evidence of bias about it

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to the randomisation process, due to deviations from the intended interventions and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignment

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations of the protocol and some concerns of risk of bias due to selection of reported results.

Kaser 2017

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

The observed number of events is much greater than the number of participants with missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote:"NCT02218255"

There are some concerns of risk of bias due to deviations from the intended interventions.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Schillaci 2002

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Subgroup 3.4.3 randomised on day 2 to 3

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. All 118 randomised women were analysed.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All ranomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Kaur 2014

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Singh 2017

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealment and no information about the baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

It is not possible to know if there were missing outcome data.

Method of measuring the outcome was not informed, but it was probably not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is a high risk of bias due to deviations from the intended interventions and missing outcomes data. And some concerns of risk of bias due to randomisation process and selection of reported results.

Ten 2011

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the analysis that was performed.

No information about neither the absolute number of events nor the missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and missing outcomes, and some concerns of risk of bias due to randomisation process and selection of reported results.

Subgroup 3.4.4 day of randomisation unstated

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Gaafar 2015

Low risk of bias Some concerns High risk of bias Low risk of bias Some concerns Some concerns

Quote "Randomization was done by computer permuted blocks size of 4, allocation by closed envelops, parallel technique" No mention about opaque envelopes

Not evidence of potential of concerns generating a substantial impact

A large proportion of missing outcomes: 326 were eligible. 126 cases had day 2/3 transfer and 126 had blastocyst transfer.

Clinical pregnancy with cardiac pulsation four weeks after ET. PACTR201308000581376 Quote "Masking Care giver/Provider,Outcome assessors,Participants"

There is only a difference in outcome reporting regarding multiple pregnancies

High bias due to missing outcome data and some concerns due to deviations from intended interventions and bias in selection of the reported result

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Pantos 2004

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

There is no information about the method of measuring the outcome, but it is probable that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 3.4 Clinical pregnancy rate per couple: grouped by day of randomisation
Risk of bias for analysis 3.5 Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Kaser 2017

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

The observed number of events is much greater than the number of participants with missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote:"NCT02218255"

There are some concerns of risk of bias due to deviations from the intended interventions.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Figuras y tablas -
Risk of bias for analysis 3.5 Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage
Risk of bias for analysis 3.6 Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus TLS (with algorithm) blastocyst stage

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Kaser 2017

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

The observed number of events is much greater than the number of participants with missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote:"NCT02218255"

There are some concerns of risk of bias due to deviations from the intended interventions.

Figuras y tablas -
Risk of bias for analysis 3.6 Clinical pregnancy rate per couple: TLS (with algorithm) cleavage stage versus TLS (with algorithm) blastocyst stage
Risk of bias for analysis 4.1 Multiple pregnancy rate per couple

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All ranomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignement

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Kaur 2014

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to the randomisation process and deviations from the intended interventions, and some concerns of risk of bias due to selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalized before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Figuras y tablas -
Risk of bias for analysis 4.1 Multiple pregnancy rate per couple
Risk of bias for analysis 4.2 Multiple pregnancy rate per couple: grouped by number of embryos transferred

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 4.2.1 equal number of embryos transferred

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignement

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Kaur 2014

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to deviations from the intended interventions and randomisation process, and some concerns of risk of bias due to selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalized before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Subgroup 4.2.2 more cleavage stage than blastocyst embryos transferred

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All ranomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations of the protocol and some concerns of risk of bias due to selection of reported results.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Subgroup 4.2.3 single embryo transfer

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Figuras y tablas -
Risk of bias for analysis 4.2 Multiple pregnancy rate per couple: grouped by number of embryos transferred
Risk of bias for analysis 4.3 Multiple pregnancy rate per couple: grouped by prognosis

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 4.3.1 good prognostic factors

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All ranomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignement

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Kaur 2014

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalized before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Subgroup 4.3.2 poor prognostic factors

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Subgroup 4.3.3 unselected

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to deviations from the intended interventions and randomisation process, and some concerns of risk of bias due to selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 4.3 Multiple pregnancy rate per couple: grouped by prognosis
Risk of bias for analysis 4.4 Multiple pregnancy rate per couple: grouped by day of randomisation

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Subgroup 4.4.1 randomised start of cycle

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignement

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to deviations from the intended interventions and randomisation process, and some concerns of risk of bias due to selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalized before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Subgroup 4.4.2 randomised on day of OPU or day 1

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations of the protocol and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Subgroup 4.4.3 randomised on day 2 to 3

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All ranomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Kaur 2014

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Subgroup 4.4.4 day of randomisation unstated

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 4.4 Multiple pregnancy rate per couple: grouped by day of randomisation
Risk of bias for analysis 4.5 High‐order pregnancies (more than 2 gestational sacs) per couple

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignement

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Kaur 2014

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to randomisation process, deviations from the intended interventions, and some concerns of risk of bias due to selection of reported results.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 4.5 High‐order pregnancies (more than 2 gestational sacs) per couple
Risk of bias for analysis 4.6 Multiple pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Figuras y tablas -
Risk of bias for analysis 4.6 Multiple pregnancy rate per couple: TLS (with algorithm) cleavage stage versus conventional blastocyst stage
Risk of bias for analysis 5.1 Miscarriage rate per couple

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to randomization process and selection of the reported result

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to the randomisation process, deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Elgindy 2011

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

The number of embryos per transfer was significantly higher in group than the other group

This open‐label, prospective, randomized, controlled trial. No information about a deviation from the intended protocols

All randomised women were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process, deviations from intended interventions and selection of reported results.

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Gaafar 2015

Low risk of bias Some concerns High risk of bias Low risk of bias Some concerns High risk of bias

Quote "Randomization was done by computer permuted blocks size of 4, allocation by closed envelops, parallel technique" No mention about opaque envelopes

Not evidence of potential of concearns generating a substantial impact

A large proportion of missing outcomes: 326 were eligible. 126 cases had day 2/3 transfer and 126 had blastocyst transfer.

PACTR201308000581376 Quote "Masking Care giver/Provider,Outcome assessors,Participants"

There is only a difference in outcome reporting regarding multiple pregnancies

High bias due to missing outcome data and some concerns due to deviations from intended interventions and bias in selection of the reported result

Hatirnaz 2017

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

95 out of 100 women of each arm had data to analyze

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignement

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Kaur 2014

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and/or concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, and selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to deviations from the intended interventions and randomisation process, and some concerns of risk of bias due to selection of reported results.

Levi‐Setti 2018

Some concerns Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was not concealed but no baseline clinical and statistical differences between groups were found in a table that described more than 15 different variables.

Participants and embryologists were aware of their assigned intervention. No deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

No lost to follow up

Method of measuring the outcome was not informed. However, given the nature of the outcome and the methods to measure it, it was probably not different between groups and, as it is an objective outcome, it is unlikely to be influenced by the knowledge of the assigned intervention.

Data that produced this result was analysed in accordance with a pre‐specified analysis plan that was finalized before unblinded outcome data were available for analysis

There is some concerns of risk of bias due to randomisation process.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Livingstone 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Yang 2018

Low risk of bias Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns

Allocation sequence was random and concealed

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the number of randomised women per arm and it is not possible to know how the analysis was performed.

The observed number of events is much greater than the number of participants with missing outcome data, but it is probably not related with the true value

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

Quote" ChiCTR‐ICR‐15006600"

There are some concerns of risk of bias due to deviations from the intended interventions.

Figuras y tablas -
Risk of bias for analysis 5.1 Miscarriage rate per couple
Risk of bias for analysis 6.1 Embryo freezing per couple

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Brugnon 2010

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

Sequence generated but there was no information about concealment. No table of patients' baseline characteristics reported

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No information about the deviations or the analysis

No information. Only proportions were reported

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk due to deviation from the intended interventions

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. All 118 randomised women were analysed.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Fernandez‐Shaw 2015

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No statement about allocation concealment.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Method of measuring the outcome was probably appropriate, in both groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Gardner 1998a

Some concerns High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

Concealment was not reported, there was a difference in Previous no. of cycles

No effort for blindness is described. There was a difference No. of embryos transferred and proportion of embryo freezing that likely have affected the outcome

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

ClinicalTrials.gov Identifier: NCT03764865

High risk of bias due to deviations from intended intervention

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignement

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to deviations from the intended interventions and randomisation process, and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Pantos 2004

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

There is no information about the method of measuring the outcome, but it is probable that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Ten 2011

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. And no information about the analysis that was performed.

No information about neither the absolute number of events nor the missing outcome data.

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and missing outcomes, and some concerns of risk of bias due to randomisation process and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 6.1 Embryo freezing per couple
Risk of bias for analysis 7.1 Failure to transfer any embryos (per couple)

Bias

Study

Randomisation process

Deviations from intended interventions

Missing outcome data

Measurement of the outcome

Selection of the reported results

Overall

Gardner 1998a

Some concerns High risk of bias Low risk of bias Low risk of bias Low risk of bias High risk of bias

Concealment was not reported, there was a difference in Previous no. of cycles

No effort for blindness is described. There was a difference No. of embryos transferred and proportion of embryo freezing that likely have affected the outcome

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

ClinicalTrials.gov Identifier: NCT03764865

High risk of bias due to deviations from intended intervention

Aziminekoo 2015

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All 118 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Bungum 2003

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not a complete explanation about concealment and there are some concerns about baseline differences

No effort for blindness is described. All 118 randomised women were analysed.

All 118 randomised women were analysed.

Method of measuring the outcome was probably appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results

Coskun 2000

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

Randomisation process apparently has no problems. Patients were randomized to receive embryo transfer either at day 3 or day 5. Quote " An equal number of ‘day 3' or ‘day 5' labels placed in sealed envelopes in a block of 14 was kept in a box and an envelope was drawn by the embryologist as soon as a patient qualified for the study. The label was attached with adhesive to the patients’ data collection sheet."

Participants and carers and people delivering the intervention were probably aware of their assigned intervention.

All 201 randomised women were available.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

Some concerns due to deviation from intended interventions and selection of reported outcomes

Devreker 2000

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidencesuggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions and there are some concerns of risk of bias due to the selection of reported results.

Emiliani 2003

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Concealment was not stated. Only minor differences in age

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention.

All women randomised were analysed

Not reported but inappropriate methotds are unlikely. It is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention

No protocol registration was found.

There some concerns of risk of bias due to the randomisation process and selection of reported results.

Frattarelli 2003

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Randomization was accomplished using a computer‐generated randomization table. The sequences of randomization were concealed until intervention was assigned. The groups were balanced. Concealment method was not described.

Those patients undergoing a day 5 ET had a significantly higher implantation rate than those undergoing a day 3, these deviations likely have affected the outcome

All women randomised were analysed

Method of measuring the outcome was probably appropriate, no different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

High risk of bias due to deviations from the intended protocol and some concerns due to bias in selection of the reported result.

Hreinsson 2004

Low risk of bias Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

Allocation sequence was random and concealed. Quote:"Sealed envelopes were used for randomisation of the patients for each group". Groups were balanced.

No effort for blindness is described. Considering the nature of the intervention, it is very unlikely that participants and carers and people delivering the intervention were not aware of their assigned intervention. No differences in embryos per transfer bat there was for cycles with embryo freezing. All women randomised were analyses by assignement

All women randomised were analysed

Knowledge of the assigned intervention is unlikely to influence this objective outcome assessment.

No protocol registration was found.

Some concerns of risk of bias due to selection of reported results.

Karaki 2002

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information if the allocation sequence was random, but it was concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. All randomised women were analysed.

No missing outcome data.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Kolibianakis 2004

High risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random but it was not concealed. No baseline differences between groups were found.

Participants, carers and people delivering the intervention were aware of their assigned intervention. No information about a deviation from the intended protocols. No information if there was a substantial impact of the failure to analyse participants in the group to which they were randomized.

All randomised women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are high of risk of bias due to deviations from the intended interventions and randomisation process, and some concerns of risk of bias due to selection of reported results.

Levitas 2004

Low risk of bias High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

Allocation sequence was random and concealed and no baseline differences were found between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was probably a deviation from the intended protocols. Analysis was done by ITT

Although there are missing outcome data, the missingness in the outcome probably does not depend on its true value.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to devitations of the protocol and some concerns of risk of bias due to selection of reported results.

Levron 2002

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

No information if the allocation sequence was random and concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. Analysis was performed by intention‐to‐treat.

Only 3 out of 46 in the blastocyst group did not have embryo transfer

Method of measuring the outcome was not stated, but it is not probable that it was measured different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Motta 1998

Some concerns High risk of bias Low risk of bias Low risk of bias Some concerns High risk of bias

No information available to know if the allocation sequence was random or the allocation sequence was concealed. And no information about baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There was evidence suggesting deviation from the intended protocols. All randomised women were analysed.

No lost to follow up

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to the randomisation process, deviations from the intended interventions and there are some concerns of risk of bias due to the randomisation process and selection of reported results.

Papanikolaou 2005

Some concerns Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed.

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process, deviations from the intended interventions and selection of reported results.

Papanikolaou 2006

Some concerns Low risk of bias Low risk of bias Low risk of bias Some concerns Some concerns

There was not enough information to evaluate the method of allocation sequence concealment.

Participants were probably aware of their assigned intervention. No deviation from the intended protocols. All randomised women were analysed.

All the randomized women were analysed

Method of measuring the outcome was appropriate, was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to randomisation process and selection of reported results.

Rienzi 2002

Some concerns High risk of bias High risk of bias Low risk of bias Some concerns High risk of bias

No information about the allocation sequence concealed but no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. No information about a deviation from the intended protocols and no information about the total number of randomised women.

No information about neither the total number of randomized women nor the missing outcome data.

Method of measuring the outcome was appropriate, it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There is high risk of bias due to deviations from the intended interventions, and there are some concerns of risk of bias due to randomisation process, missing outcomes and selection of reported results.

Van der Auwera 2002

Low risk of bias Some concerns Low risk of bias Low risk of bias Some concerns Some concerns

No information available to know if the allocation sequence was random. However, allocation sequence was concealed and no baseline differences between groups.

Participants, carers and people delivering the intervention were probably aware of their assigned intervention. There were only few with deviation from the intended protocols, and no imbalance was found. All randomised women were analysed.

Quote: “Three patients were excluded for analysis from group 1 because they wanted an elective blastocyst culture while four patients were excluded from group 2 because they wanted an elective day 2 transfer.”

Method of measuring the outcome was not described. However, it is unlikely that it was not different between groups and it is an objective outcome that is unlikely to be influenced by the knowledge of the assigned intervention.

No protocol registration was found.

There are some concerns of risk of bias due to deviations from the intended interventions and selection of reported results.

Figuras y tablas -
Risk of bias for analysis 7.1 Failure to transfer any embryos (per couple)