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تاثیر مکمل گلوتامین در کودکان خردسال مبتلا به بیماری شدید گوارشی

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پیشینه

بیوسنتز درون‌زای گلوتامین ممکن است برای رفع نیازهای بیماران مبتلا به بیماری شدید گوارشی کافی نباشد. نتایج مطالعات آزمایشی که از مدل‌های حیوانی بیماری‌های گوارشی استفاده کردند، نشان داده‌اند که مکمل گلوتامین پیامدهای بالینی بیماری را بهبود می‌بخشد. این مرور، شواهدی را در مورد تاثیر مصرف مکمل گلوتامین در کودکان خردسال مبتلا به بیماری شدید گوارشی بررسی می‌کند.

اهداف

ارزیابی تاثیر مکمل گلوتامین بر مورتالیتی و موربیدیتی در کودکان خردسال مبتلا به بیماری شدید گوارشی.

روش‌های جست‌وجو

این جست‌وجو شامل پایگاه مرکزی ثبت کارآزمایی‌های کنترل شده کاکرین (CENTRAL) (کتابخانه کاکرین؛ 2014، شماره 8)؛ MEDLINE؛ EMBASE و CINAHL (از ابتدا تا سپتامبر ‌2014)؛ خلاصه مقالات کنفرانس‌ها، و مرورهای قبلی بود.

معیارهای انتخاب

کارآزمایی‌های تصادفی‌سازی‌شده یا شبه تصادفی‌سازی‌شده و‌کنترل شده که مکمل گلوتامین را با عدم مصرف آن در نوزادان تا سه ماهگی (در صورت لزوم برای زایمان زودرس اصلاح شد) و مبتلا به بیماری شدید گوارشی مقایسه کردند که به عنوان یک بیماری گوارشی مادرزادی یا اکتسابی تعریف شد که حداقل به مدت 24 ساعت به تغذیه وریدی نیاز داشتند.

گردآوری و تجزیه‌وتحلیل داده‌ها

دو نویسنده مرور، واجد شرایط بودن کارآزمایی و خطر سوگیری (bias) را ارزیابی کرده و به‌طور مستقل از هم استخراج داده‌ها را انجام دادند. تاثیرات درمان را در کارآزمایی‌های فردی آنالیز کرده و خطر نسبی (RR) و تفاوت خطر (risk difference) را برای داده‌های دو حالتی (dichotomous) و تفاوت میانگین (MD) را برای داده‌‏های پیوسته (continuous data)، با 95% فاصله اطمینان (CI)، گزارش کردیم. از یک مدل اثر ثابت در متاآنالیزها استفاده کرده و علل بالقوه ناهمگونی را در آنالیزهای حساسیت (sensitivity) بررسی کردیم.

نتایج اصلی

سه کارآزمایی را پیدا کردیم که در مجموع 274 نوزاد در آنها شرکت کردند. کیفیت روش‌شناسی (methodology) کارآزمایی‌ها خوب بود، اما برای تشخیص تاثیرات مهم بالینی مکمل گلوتامین بسیار کوچک بودند. متاآنالیزها تفاوت آماری معنی‌داری را در خطر مرگ‌ومیر پیش از ترخیص از بیمارستان (RR معمول: 0.79؛ 95% CI؛ 0.19 تا 3.20؛ RD معمول: 0.01‐؛ 95% CI؛ 0.05‐ تا 0.03) یا در نرخ بروز عفونت تهاجمی (RR معمول: 1.37؛ 95% CI؛ 0.89 تا 2.11؛ RD معمول: 0.08، 95% CI ‐0.03 تا 0.18) نشان ندادند.

نتیجه‌گیری‌های نویسندگان

داده‌های موجود از کارآزمایی‌های تصادفی‌سازی و کنترل شده نشان نمی‌دهند که مکمل‌های گلوتامین مزایای مهمی برای کودکان خردسال مبتلا به بیماری شدید گوارشی دارند.

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.

خلاصه به زبان ساده

تاثیر مکمل گلوتامین در کودکان خردسال مبتلا به بیماری شدید گوارشی

گلوتامین یک اسید آمینه است که به بافت‌ها، به‌ویژه در دستگاه گوارش، کمک می‌کند تا پس از آسیب بهبود پیدا کنند. ما به دنبال شواهدی بودیم که نشان دهد مصرف گلوتامین اضافی توسط کودکان خردسال مبتلا به مشکلات شدید روده، به آنها کمک می‌کند تا سریع‌تر و کامل‌تر بهبود یابند یا خیر. در حال حاضر، فقط سه کارآزمایی در دسترس هستند؛ نتایج نشان می‌دهند که مکمل گلوتامین هیچ فایده‌ای برای این نوزادان ندارد.

Authors' conclusions

Implications for practice

The currently available evidence from three trials does not indicate that glutamine supplementation improves important clinical outcomes for young infants with severe gastrointestinal disease.

Implications for research

A very large randomised controlled trial is required to assess whether glutamine supplementation is beneficial for young infants with severe gastrointestinal disease. Future trials may also need to be of sufficient size to allow subgroup analyses by type of gastrointestinal disease and by gestational age.

Background

Description of the condition

Severe gastrointestinal disease ‐ including acute necrotising enterocolitis (NEC), spontaneous localised intestinal perforation, congenital gut anomalies and atresias, anterior abdominal wall defects, Hirschsprung's disease, and acute malrotation or volvulus ‐ is an important cause of morbidity, mortality and neuro‐disability in newborn and young infants (Kays 1996; Hajivassiliou 2003). Infants with severe gastrointestinal disease experience more episodes of invasive infection, have lower levels of nutrient intake, grow more slowly, and have longer duration of intensive care and hospital stay than gestation‐comparable infants without gastrointestinal disease (Dalla Vecchia 1998; Donnell 2002; Abdullah 2007). Severe NEC, especially if treated surgically, is associated with a higher rate of long‐term neurological disability, which may be a consequence of infection and under‐nutrition during a critical period of brain development (Stoll 2004; Rees 2007).

Description of the intervention

Glutamine is a key source of energy for rapidly dividing cells such as enterocytes, lymphocytes, macrophages, and neutrophils (Windmueller 1980; Newsholme 1999). Although glutamine can be synthesised in vivo, it is considered a 'conditionally essential' amino acid in catabolic states, where demand outstrips supply (Lacey 1990). Plasma glutamine levels fall during critical illness or following major surgery and glutamine deficiency may limit tissue recovery in these situations (Parry‐Billings 1990; Parry‐Billings 1992; Newsholme 2001). While glutamine is present in human breast milk, infant formula is low in glutamine, and standard parenteral nutrition solutions contain no glutamine because it is not stable in an aqueous environment (Khan 1991; Agostini 2000). Thus, infants who have severe gastrointestinal disease or who are recovering from major gastrointestinal surgery are unlikely to receive sufficient glutamine. Synthetic glutamine‐containing dipeptides that are stable in aqueous solution are available, however (Furst 1997). It is therefore feasible to provide supplemental glutamine to infants with these conditions.

In theory, glutamine supplementation may confer several benefits to young infants with severe gastrointestinal disease. Accelerating anastomosis and wound healing and enhancing gut mucosal integrity might help infants to tolerate enteral feeding earlier and thereby shorten their duration of hospitalisation. In fact, improving gut barrier function and lymphocyte production may reduce the rate of acquired infection, lower mortality, and in the longer term, lower rates of adverse neurodevelopmental outcomes.

How the intervention might work

In experimental animal models of enterocolitis, providing supplemental glutamine aided gut recovery, probably by providing additional energy for enterocyte division and proliferation (Klimberg 1990; Rombeau 1990). Peri‐ or postoperative glutamine supplementation may also accelerate bowel anastomosis healing (McCauley 1991; da Costa 2003). In adult surgical or critically ill patients, some evidence exists that glutamine supplementation preserves gut mucosal integrity and reduces infectious complications and (possibly) mortality (Van der Hulst 1993; Novak 2002; Estivariz 2008). However, concerns about trial quality and publication bias have limited the reliability and applicability of these findings (Avenell 2009; Murray 2009). More recent, larger and better quality trials have failed to demonstrate clinically important benefits of glutamine supplementation in this population (Andrews 2011).

There is a theoretical concern that supplemental glutamine, via its metabolic products glutamate and ammonia, may have adverse neurological effects in high concentrations (Garlick 2001). However, metabolic studies in preterm infants have found that parenteral glutamine supplementation (up to 0.6 g/kg/day) limits whole body proteolysis without increasing plasma amino acid or ammonia levels (Kalhan 2005). Enterally administered glutamine is metabolised entirely in the splanchnic compartment and does not affect whole‐body ammonia or urea nitrogen levels (Parimi 2004). Systematic reviews have not found evidence of adverse effects of glutamine supplementation in adults or in clinically stable preterm infants (Novak 2002; Avenell 2009; Murray 2009; Moe‐Byrne 2012).

Why it is important to do this review

A previous Cochrane review on routine glutamine supplementation for preterm infants concluded that there is no evidence of any benefits or harms (Moe‐Byrne 2012). Although the infants who participated in these trials were all of very low birth weight, most were clinically stable. Any putative benefits of glutamine supplementation might be confined to critically ill infants for whom glutamine availability is rate‐limiting for tissue repair, for example, infants with severe gastrointestinal disease such as NEC or infants who have undergone major gastrointestinal surgery (Pierro 2002).

Objectives

To determine whether supplemental glutamine for infants with severe gastrointestinal disease reduces mortality, decreases the time taken to establish enteral feeding, reduces the incidence of late‐onset invasive infection, shortens the duration of hospitalisation, increases growth rates, and prevents adverse neurodevelopmental outcomes.

Methods

Criteria for considering studies for this review

Types of studies

Controlled trials using either random or quasi‐random patient allocation.

Types of participants

Newborn and young infants (up to and including three months old, corrected for preterm birth) with severe gastrointestinal disease defined as a congenital or acquired gastrointestinal condition that is likely to necessitate parenteral nutrition; for example, NEC, anterior abdominal wall defect, or intestinal obstruction. Infants should have been enrolled to participate in the trial within one week after gastrointestinal surgery or after the onset of NEC (if treated non‐surgically).

NEC should have been diagnosed using Bell's criteria or modifications, that is, the presence of at least two of the following features: pneumatosis coli on abdominal radiograph; abdominal distension or abdominal radiograph with gaseous distension or frothy appearance of bowel lumen (or both); blood in stool; and lethargy, hypotonia, or apnoea, or combination of these (Bell 1978; Walsh 1986).

Types of interventions

Glutamine supplementation versus no supplementation or placebo by the parenteral or enteral route. We did not pre‐specify a minimum duration of intervention.

Types of outcome measures

Primary outcomes

  1. Death prior to hospital discharge.

  2. Neurodevelopmental outcomes assessed beyond infancy (neurological evaluations, developmental scores, and classifications of disability including auditory and visual disability, non‐ambulant cerebral palsy, and developmental delay) and cognitive and educational outcomes (intelligence quotient and/or indices of educational achievement measured using a validated tool, including school examination results).

Secondary outcomes

  1. Time from trial entry to establish full enteral feeds independent of parenteral fluids or nutrition.

  2. Incidence of invasive infection during hospital admission as determined by culture of bacteria or fungus from blood, cerebrospinal fluid, urine, or from a normally sterile body space (number of participants per group with one or more episodes).

  3. Time from trial entry to discharge from hospital.

  4. Growth during the trial period: weight gain (g/day or g/kg/day), linear growth (mm/week), head growth (mm/week), and skinfold thickness growth (mm/week).

Search methods for identification of studies

We used the standard search strategy of the Cochrane Neonatal Review Group.

Electronic searches

An update search was carried out in September 2014 to locate randomised controlled trials of glutamine supplementation in surgical infants since the date of the last search in November 2011.

We searched the Cochrane Central Register of Controlled Trials (CENTRAL) (Wiley), EMBASE (OvidSP), Maternity and Infant Care (OvidSP), MEDLINE & MEDLINE in process (OvidSP) and PubMed. We limited the searches to references added to the databases since November 2011. We limited retrieval to clinical trials using a search filter where possible. We did not apply language restrictions.

We searched for ongoing and completed trials in ClinicalTrials.gov, metaRegister of Controlled Trials (mRCT), and the World Health Orgainzation International Clinical Trials Registry Platform (ICTRP), limiting where possible to trials added or updated since November 2011.

Full search strategies with results can be found in Appendix 1.

Searching other resources

We examined the reference lists of studies identified as potentially relevant. We searched the abstracts from the annual meetings of the Pediatric Academic Societies (1993 to 2014), the European Society for Paediatric Research (1995 to 2013), the UK Royal College of Paediatrics and Child Health (2000 to 2014), and the Perinatal Society of Australia and New Zealand (2000 to 2014). We considered trials reported only as abstracts to be eligible if sufficient information was available from the report, or from contact with the authors, to fulfil the inclusion criteria.

Data collection and analysis

We used the standard methods of the Cochrane Neonatal Review Group.

Selection of studies

Two review authors screened the title and abstract of all studies identified by the above search strategy. We assessed the full text of any potentially eligible reports and excluded those studies that did not meet all of the inclusion criteria. We discussed any disagreements until consensus was achieved.

Data extraction and management

We used a data collection form to aid extraction of relevant information from each included study. Two review authors extracted the data separately. We discussed any disagreements until consensus was achieved. We asked the investigators for further information if data from the trial reports were insufficient.

Assessment of risk of bias in included studies

We used the criteria and standard methods of the Cochrane Neonatal Review Group to assess the methodological quality of any included trials. Additional information from the trial authors was requested to clarify methodology and results as necessary. We evaluated and reported the following issues in the 'Risk of bias' tables.

  1. Sequence generation: we categorised the method used to generate the allocation sequence as:

    1. low risk: any random process (e.g. random number table; computer random number generator);

    2. high risk: any non‐random process (e.g. odd or even date of birth; patient case‐record number);

    3. unclear.

  2. Allocation concealment: we categorised the method used to conceal the allocation sequence as:

    1. low risk: (e.g. telephone or central randomisation; consecutively numbered sealed opaque envelopes);

    2. high risk: open random allocation; unsealed or non‐opaque envelopes, alternation; date of birth;

    3. unclear.

  3. Blinding: we assessed blinding of participants, clinicians and carers, and outcome assessors separately for different outcomes and categorised the methods as:

    1. low risk;

    2. high risk;

    3. unclear.

  4. Incomplete outcome data: we described the completeness of data including attrition and exclusions from the analysis for each outcome and any reasons for attrition or exclusion where reported. We assessed whether missing data were balanced across groups or were related to outcomes. Where sufficient information was reported or supplied by the trial authors, we re‐included missing data in the analyses. We categorised completeness as:

    1. low risk: < 20% missing data;

    2. high risk: ≥ 20% missing data;

    3. unclear.

Measures of treatment effect

We calculated risk ratio (RR) and risk difference (RD) for dichotomous data and weighted mean difference (WMD) for continuous data with respective 95% confidence intervals (CI). We determined the number needed to treat for benefit (NNTB) or harm (NNTH) for a statistically significant difference in the RD.

Unit of analysis issues

The unit of analysis is the participating infant in individually randomised trials and the neonatal unit for cluster randomised trials.

Dealing with missing data

We requested missing study data from the trial investigators.

Assessment of heterogeneity

If more than one trial was included in a meta‐analysis, we examined the treatment effects of individual trials and heterogeneity between trial results by inspecting the forest plots. We calculated the I² statistic for each analysis to quantify inconsistency across studies and describe the percentage of variability in effect estimates that may be due to heterogeneity rather than sampling error. If substantial (I² > 50%) heterogeneity was detected, we explored the possible causes (for example, differences in study design, participants, interventions, or completeness of outcome assessments) in sensitivity analyses.

Data synthesis

We used a fixed‐effect model for meta‐analyses.

Subgroup analysis and investigation of heterogeneity

We pre‐specified the following subgroup analyses:

  1. trials where participants were predominantly (> 80%) term infants versus trials where participants were predominantly preterm infants;

  2. trials where participants were infants with NEC versus trials where participants were infants who had undergone gastrointestinal surgery for other indications;

  3. trials where infants received enteral glutamine supplementation versus trials where supplemental glutamine was given parenterally;

  4. trials where the aim was to give at least 0.2 g/kg/day of glutamine versus trials where less glutamine supplementation was given.

Results

Description of studies

See Characteristics of included studies; Characteristics of excluded studies.

Results of the search

We have included a trial previously identified as ongoing in this review update (Ong 2012). The status of NCT00647036, which was also identified as ongoing in 2011, is not known.

Three trials, in which a total of 274 infants participated, fulfilled eligibility criteria (Duggan 2004; Albers 2005, Ong 2012). The abstract of another small trial (n = 13) was found by our searches in 2011 (Nolin 2001). Further searching in September 2014 identified the full‐text of a master's thesis (Nolin 2000). As this study did not focus on infants undergoing gastrointestinal surgery we have now excluded it from this review.

Included studies

Two trials were single‐centre studies undertaken in surgical neonatal and paediatric intensive care centres in Europe (Albers 2005) and North America (Duggan 2004). The third trial was conducted in 14 paediatric surgical units across the UK (Ong 2012). All participants were recruited between 2000 and 2005. The smallest trial was a pilot study that aimed to assess feasibility and safety (Duggan 2004).

Participants

Duggan 2004 enrolled 20 young infants with severe gastrointestinal diseases (NEC, intestinal atresia, or anterior abdominal wall defects). Most participants were preterm (average gestational age at birth 33 weeks). Their median postnatal age at enrolment was 15 days.

Albers 2005 enrolled 80 children of gestational age at birth > 30 weeks and chronological age less than two years. This trial, therefore, did not strictly fulfil our a priori population criterion (infants < 3 months old). However, we decided to include the trial because the report stated that most (69 of the 80) participants were less than six months old at enrolment. The report did not provide subgroup data for infants less than three months old. The most common gastrointestinal conditions affecting participants were NEC, congenital bowel atresia or obstruction, anterior abdominal wall defects, and Hirschsprung's disease. Infants were not expected to be able to tolerate enteral nutrition for at least four days following gastrointestinal tract surgery. The median postnatal age at enrolment was 11 days.

Ong 2012 enrolled 174 young infants with severe gastrointestinal diseases (abdominal wall defect, congenital bowel obstruction, or NEC). Most participants were born at term (median gestational age at birth 37 weeks). Their median postnatal age at enrolment was five days.

Interventions

Duggan 2004: When judged by the attending clinicians to be ready to tolerate the introduction of enteral feeds, participating infants were randomly allocated to either glutamine‐supplemented expressed human milk or hydrolysed formula milk versus human milk or formula without added glutamine (but with an iso‐osmolar mix of non‐essential amino acids). The glutamine‐supplemented and non‐supplemented milks were indistinguishable to the parents, carers, and assessors. The intervention group received 0.08 g/kg/day of glutamine at the start of the study. This increased to 0.31 g/kg/day by two weeks post enrolment. Glutamine supplementation was stopped on day 30. All infants received the same level of parenteral nutrition (without added glutamine) while enteral feeds were being advanced.

Albers 2005: On the second postoperative day, infants in the intervention group received a standard parenteral nutrition solution supplemented with L‐glutamine sufficient to provide 0.4 g/kg/day. Control infants received parenteral nutrition with an iso‐nitrogenous amino acid solution. The carers were not aware whether participating infants received glutamine‐supplemented or non‐supplemented parenteral nutrition. The protocol specified that participating infants should continue to receive full parenteral nutrition until at least the sixth postoperative day when enteral feeding was gradually re‐introduced.

Ong 2012: From day three of parenteral nutrition, infants in the intervention group received a glutamine dipeptide supplement providing 0.4 g/kg/day of glutamine. This was continued while parenteral nutrition was administered. The control group received an isonitrogenous, isocaloric parenteral nutrition solution. The solutions were indistinguishable to parents, carers, and assessors, and nutritional information on labels did not allow identification of the solution. All study participants received only parenteral nutrition at the start of the trial and were gradually progressed to full enteral feeds. While exclusively receiving parenteral nutrition the control group did not receive any glutamine. With the introduction of enteral feeds, the control group received some naturally occurring glutamine in breast milk or formula.

Outcomes

Duggan 2004 assessed the effect of enteral glutamine supplementation on the time taken to establish full enteral feeding, rates of nosocomial infection, and growth during the study period.

Albers 2005 assessed the effect of parenteral glutamine supplementation on intestinal permeability (urinary excretion ratios of lactulose and rhamnose) and nitrogen balance. Mortality, duration of intensive care stay, and rates of nosocomial infection were reported as secondary outcomes.

Ong 2012 assessed the effect of parenteral glutamine supplementation on time required to achieve full enteral nutrition and the incidence of "sepsis" and "septicaemia". Adverse events and mortality were also reported.

Excluded studies

Three trials that appeared potentially eligible were excluded after further evaluation of the full report (Barbosa 1999; Nolin 2000, Ehrenkranz 2011). Most participants in these trials were infants with non‐gastrointestinal disease.

Risk of bias in included studies

The overall methodological quality of all studies was good.

Allocation

All trials used methods to conceal allocation.

Blinding

All trials blinded carers and assessors to the intervention.

Incomplete outcome data

All trials achieved complete or near‐complete follow‐up.

Effects of interventions

Glutamine supplementation (parenteral or enteral) versus no supplementation

Mortality prior to hospital discharge (Outcome 1.1):

None of the trials nor a meta‐analysis of data from all trials showed a statistically significant difference in mortality (typical RR 0.79, 95% CI 0.19 to 3.20; typical RD ‐0.01, 95% CI ‐0.05 to 0.03). (Figure 1; Analysis 1.1).


Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.1: death prior to hospital discharge.

Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.1: death prior to hospital discharge.

Neurodevelopmental outcomes

This outcome was not assessed in any trial.

Incidence of invasive infection (Outcome 1.2)

None of the trials nor a meta‐analysis of data from both trials showed a statistically significant difference in infection rates (typical RR 1.37, 95% CI 0.89 to 2.11; typical RD 0.08, 95% CI ‐0.03 to 0.18). (Figure 2; Analysis 1.2)


Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.2: incidence of invasive infection.

Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.2: incidence of invasive infection.

Time to establish full enteral feeds

Duggan 2004 reported no statistically significant difference in the time taken to establish full enteral feeding in the intervention group (median 39 days; interquartile range 12 to 99) versus the control group (median 21 days; interquartile range 6 to 59). Similarly, Ong 2012 reported that there was no statistically significant difference in the time taken to establish full enteral feeds between the intervention group (median: 19 days; 5th to 95th centile 14.6 to 23.4) and the control group (median: 16 days; 5th to 95th centile 13.6 to 18.4). Albers 2005 did not report on this outcome.

Time to discharge from hospital

Albers 2005 did not find a statistically significant difference between the intervention group (median 32 days; interquartile range 16.8 to 44.8) and the control group (median 31.5 days; interquartile range 14 to 64). Duggan 2004 did not assess time to hospital discharge (according to personal communication from trial authors). Time to discharge was not reported by Ong 2012.

Growth during the trial period

Duggan 2004 did not find a statistically significant difference in the rate of weight gain during the study period (MD 3.80 g/day; 95% CI ‐6.65 to 14.25) (Figure 3; Analysis 1.3). The report also stated that there was not a statistically significant difference in the rate of change in length or 'arm anthropometrics' but data were not presented. Ong 2012 reported no significant difference in weight centile change between groups and maintenance of head circumference centiles in each group. Data were not presented. Albers 2005 did not report growth during the trial period.


Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.3: weight gain during trial period (g/day).

Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.3: weight gain during trial period (g/day).

Subgroup analyses
Trials where participants were predominantly term infants versus trials where participants were predominantly preterm infants

Duggan 2004 recruited preterm infants predominantly ‐ see above. For Albers 2005 and Ong 2012, subgroup data were not available.

Trials where participants were infants with NEC versus trials where participants were infants who had undergone gastrointestinal surgery for other indications

In Albers 2005, 19 of 80 participating infants had NEC. In Duggan 2004, eight of 20 participating infants had NEC. In Ong 2012, seven of 174 participating infants had NEC. Subgroup data for infants with NEC versus other surgical gastrointestinal conditions were not presented in any of the reports.

Trials where infants received enteral glutamine supplementation versus no supplementation and trials where supplemental glutamine was given parenterally versus no supplementation

Albers 2005 and Ong 2012 studied the effect of parenteral glutamine supplementation ‐ see above. Duggan 2004 studied the effect of enteral glutamine supplementation ‐ see above.

Trials where the aim was to give at least 0.2 g/kg/day of glutamine versus trials where less glutamine supplementation was given

All trials aimed to provide at least 0.2 g/kg/day on average of glutamine.

Discussion

Summary of main results

Three good quality randomised controlled trials in which 274 infants with severe gastrointestinal disease participated assessed the effect of glutamine supplementation versus no glutamine. The available data do not provide evidence that supplemental glutamine affects mortality, rates of invasive infection, or other morbidity.

Overall completeness and applicability of evidence

Although methodologically sound, the included trials were too small to detect moderate but potentially important effects on the specified outcomes of this review. Based on a control event rate for invasive infection (consistent with the included trials), a single trial would need to enrol about 2500 participants (1250 in each group) to be able to detect a 25% risk reduction with 5% significance and 90% power. This optimum study size is an order of magnitude larger than the total number of participants in the trials identified in this review.

Furthermore, the included trials recruited a heterogeneous group of participants with a range of severe gastrointestinal diseases. This heterogeneity may limit meaningful evaluation of the effect of glutamine supplementation. For example, the effect of glutamine supplementation may be different for sick, very preterm infants recovering from severe NEC compared with term infants who have had reduction of an anterior abdominal wall defect but are otherwise metabolically and physiologically stable. If further data become available from ongoing trials, subgroup analyses by gestational age at birth (term versus preterm) or by type of gastrointestinal disease may be needed to define which groups of infants, if any, benefit from glutamine supplementation.

Variation in the route of administration of supplemental glutamine (enteral versus parenteral) is also a potentially important source of trial heterogeneity that may affect outcomes. Systematic review of trials in adults suggests that parenteral supplementation confers more clinical benefits than enteral supplementation (Novak 2002). However, laboratory studies have suggested that using the enteral route results in a much higher concentration of free glutamine being delivered to the intestinal mucosa and that this reduces bacterial translocation and invasive infection (Panigrahi 1997). The theoretical disadvantage to enteral administration is that glutamine is metabolised entirely in the splanchnic compartment with no net increase in free glutamine delivery to other organs (Parimi 2004). The most appropriate route of delivery may also be affected by the underlying gastrointestinal condition. For example, it may not be possible to deliver enteral glutamine to very preterm infants with severe NEC, but this may be the most appropriate route for clinically stable infants recovering from a less physiologically destabilising gastrointestinal condition.

Quality of the evidence

All three trials were of good methodological quality but were too small to detect moderate but potentially important effects (Duggan 2004; Albers 2005, Ong 2012).

Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.1: death prior to hospital discharge.
Figuras y tablas -
Figure 1

Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.1: death prior to hospital discharge.

Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.2: incidence of invasive infection.
Figuras y tablas -
Figure 2

Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.2: incidence of invasive infection.

Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.3: weight gain during trial period (g/day).
Figuras y tablas -
Figure 3

Forest plot of comparison 1: glutamine supplementation (parenteral or enteral) versus no supplementation, outcome 1.3: weight gain during trial period (g/day).

Comparison 1 Glutamine supplementation (parenteral or enteral) versus no supplementation, Outcome 1 Death prior to hospital discharge.
Figuras y tablas -
Analysis 1.1

Comparison 1 Glutamine supplementation (parenteral or enteral) versus no supplementation, Outcome 1 Death prior to hospital discharge.

Comparison 1 Glutamine supplementation (parenteral or enteral) versus no supplementation, Outcome 2 Incidence of invasive infection.
Figuras y tablas -
Analysis 1.2

Comparison 1 Glutamine supplementation (parenteral or enteral) versus no supplementation, Outcome 2 Incidence of invasive infection.

Comparison 1 Glutamine supplementation (parenteral or enteral) versus no supplementation, Outcome 3 Weight gain during trial period (g/day).
Figuras y tablas -
Analysis 1.3

Comparison 1 Glutamine supplementation (parenteral or enteral) versus no supplementation, Outcome 3 Weight gain during trial period (g/day).

Comparison 1. Glutamine supplementation (parenteral or enteral) versus no supplementation

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

1 Death prior to hospital discharge Show forest plot

3

263

Risk Ratio (M‐H, Fixed, 95% CI)

0.79 [0.19, 3.20]

2 Incidence of invasive infection Show forest plot

3

263

Risk Ratio (M‐H, Fixed, 95% CI)

1.37 [0.89, 2.11]

3 Weight gain during trial period (g/day) Show forest plot

1

20

Mean Difference (IV, Fixed, 95% CI)

3.80 [‐6.65, 14.25]

Figuras y tablas -
Comparison 1. Glutamine supplementation (parenteral or enteral) versus no supplementation