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Intervenciones para el tratamiento de la colestasis intrahepática en pacientes con anemia de células falciformes

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Resumen

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Antecedentes

La anemia de células falciformes es la hemoglobinopatía más común en todo el mundo, y la colestasis intrahepática de células falciformes es una complicación ampliamente reconocida en esta población. Las hepatopatías colestásicas se caracterizan por el deterioro en la formación o la excreción (o ambas) de bilis por parte del hígado. Es necesario evaluar los efectos clínicos beneficiosos y perjudiciales de las intervenciones utilizadas para tratar la colestasis intrahepática en pacientes con anemia de células falciformes. Ésta es una actualización de una revisión Cochrane publicada anteriormente.

Objetivos

Evaluar los efectos beneficiosos y perjudiciales de las intervenciones para el tratamiento de la colestasis intrahepática en pacientes con anemia de células falciformes.

Métodos de búsqueda

Se hicieron búsquedas en el registro de ensayos de Hemoglobinopatías del Grupo Cochrane de Fibrosis Quística y Enfermedades Genéticas (Cystic Fibrosis and Genetic Disorders Group's Haemoglobinopathies Trials Register), que comprende las referencias identificadas mediante búsquedas exhaustivas en bases de datos electrónicas y búsqueda manual en revistas relevantes y en libros de resúmenes de congresos. También se realizaron búsquedas en la base de datos LILACS (1982 al 23 de mayo de 2017), en el portal de búsqueda de la Plataforma de Registro Internacional de Ensayos Clínicos de la OMS (23 de mayo de 2017) y en ClinicalTrials.gov.

Fecha de la última búsqueda en el registro de ensayos de Hemoglobinopatías del Grupo Cochrane de Fibrosis Quística y Enfermedades Genéticas: 12 de abril de 2017.

Criterios de selección

Se buscaron ensayos controlados aleatorizados publicados y no publicados.

Obtención y análisis de los datos

Cada autor se propuso extraer los datos de manera independiente y evaluar el riesgo de sesgo de los ensayos mediante las metodologías estándar de Cochrane; sin embargo, no se incluyó ningún ensayo en la revisión.

Resultados principales

No se identificaron ensayos controlados aleatorizados.

Conclusiones de los autores

Esta Revisión Cochrane no identificó ensayos controlados aleatorizados que evaluaran las intervenciones para el tratamiento de la colestasis intrahepática en pacientes con anemia de células falciformes. Se necesitan ensayos controlados aleatorizados para establecer el tratamiento óptimo de esta enfermedad.

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.

Resumen en términos sencillos

Intervenciones para el tratamiento de la colestasis intrahepática en pacientes con anemia de células falciformes

Pregunta de la revisión

El objetivo fue examinar la evidencia sobre el tratamiento de la colestasis intrahepática (enfermedades hepáticas en las que la bilis no se produce o no se excreta de manera adecuada [o ambas]) en pacientes con anemia de células falciformes. Ésta es una actualización de una revisión Cochrane publicada anteriormente.

Antecedentes

La anemia de células falciformes es un trastorno hereditario y es la hemoglobinopatía más común en todo el mundo. En 2006 la OMS declaró que la anemia de células falciformes es un problema de salud pública significativo, y se calcula que un 70% de los enfermos residen en África. Es común entre las personas de ascendencia subsahariana, india, de Oriente Medio o mediterránea.

La anemia de células falciformes afecta el sistema hepatobiliar (hígado, vesícula biliar, conductos biliares), y se observa una reducción repetida del flujo sanguíneo y la formación de cálculos de bilirrubina (un tipo de cálculo biliar). Lo anterior es resultado de las células falciformes que bloquean los vasos sanguíneos y de una reducción en la duración de la vida de estas células. La colestasis intrahepática de células falciformes o hepatopatía de células falciformes (hígado anormal o enfermo) es una complicación de la enfermedad. Cuando se diagnostica, las personas con este trastorno pueden mostrar un color amarillo intenso en la piel y los ojos debido a un mayor nivel de bilirrubina en suero (ictericia), cansancio, picazón generalizada, aumento del dolor en el cuadrante superior derecho del abdomen debido a los cálculos biliares, aumento en el tamaño del hígado y niveles inferiores de hemoglobina.

La colestasis intrahepática de células falciformes, aunque poco frecuente, es una complicación potencialmente mortal con una alta tasa de mortalidad. No existe un acuerdo en cuanto a cómo diagnosticar o tratar este trastorno. Se buscó evaluar los efectos beneficiosos y perjudiciales de los tratamientos para la colestasis intrahepática en pacientes con anemia de células falciformes.

Fecha de la búsqueda

La evidencia está actualizada hasta el 12 de abril de 2017.

Características de los estudios

No su pudo encontrar ningún ensayo elegible.

Resultados clave

No se identificaron ensayos.

Calidad de la evidencia

No existe evidencia de ensayos controlados aleatorizados de cualquier intervención para el tratamiento de la colestasis intrahepática en pacientes con anemia de células falciformes. Se necesitan ensayos para establecer el mejor tratamiento para esta enfermedad.

Authors' conclusions

Implications for practice

This update Cochrane Review identified no RCTs of non‐pharmaceutical interventions (simple red blood cell transfusion, exchange transfusion and liver transplantation) or pharmaceutical interventions (bile acid‐binding resins (i.e., cholestyramine, colestipol); rifampin; opiate antagonists (naltrexone and nalmefene); sertraline; dexamethasone; guar gum; and activated charcoal) for treating intrahepatic cholestasis in SCD. Therefore, it is not possible to determine whether any of those interventions are beneficial or harmful for people with SCD and intrahepatic cholestasis. Accordingly, we are unable to evaluate the effects of any intervention for treating intrahepatic cholestasis in SCD.

Implications for research

This update Cochrane Review has identified the need for well‐designed, adequately powered RCTs to assess the benefits and harms of non‐pharmaceutical and pharmaceutical treatments as a way of treating the intrahepatic cholestasis affecting people with SCD. Potential trials should assess clinical outcomes such as all‐cause mortality, health‐related quality of life, fatigue and adverse events. However, this is a relatively rare complication of SCD, making it unlikely that there would be enough participants to conduct such a trial in a reasonable time‐frame.

RCTs should be reported according to the consolidated standards of reporting trials (CONSORT) statement for improving the quality of reporting of efficacy and harms in clinical research (Ioannidis 2004; Moher 2010; Turner 2012). Future trials should be planned following the Standard Protocol Items: Recommendations for Interventional Trials (SPIRIT) (Chan 2013; Chan 2013a) and the Foundation of Patient‐Centered Outcomes Research recommendations (Basch 2012; Gabriel 2012; PCORI 2012).

Background

Please refer to the medical glossary (Appendix 1).

Description of the condition

Sickle cell disease (SCD) is an inherited condition and the most common hemoglobinopathy occurring worldwide (Azar 2017; Piel 2017; Ware 2017). The sickle hemoglobin is an abnormal hemoglobin due to a point mutation of the beta (β) globin gene resulting in the substitution of glutamic acid by valine at position 6 of the β globin polypeptide chain (Azar 2017; Piel 2017; Ware 2017).

According to the WHO, SCD is a major public health problem (WHO 2006; Modell 2008) with an estimated 70% of sufferers living in Africa (Tluway 2017). It is common among people with sub‐Saharan African, Indian, Middle Eastern or Mediterranean ancestry (Creary 2007; Modell 2008). The term SCD includes sickle cell anaemia (Hb SS), hemoglobin S combined with hemoglobin C (Hb SC), hemoglobin S associated with β thalassemia (Sβ0 Thal and Sβ⁺Thal) and other less prevalent double heterozygous conditions which cause clinical disease (Steinberg 2009; Weatherall 2006). Hemoglobin S combined with normal hemoglobin (A) is known as the sickle cell trait (AS), which is generally asymptomatic and is not part of this review. Recently, the clinical and other aspects of SCD have been reviewed (Azar 2017; Piel 2017; Ware 2017).

Sickle cell intrahepatic cholestasis is a hepatic complication long recognized in people with SCD (Im 2015; Malik 2015; NIH 2014; Yawn 2014) and it is considered as an medical emergency (Simon 2016). The cholestatic liver diseases are uncommon conditions characterized by impaired formation or excretion (or both) of bile from the liver. Sickle cell disease affects the hepatobiliary system (Ballas 2012; Ebert 2010), with recurrent ischemia and bilirubin stones resulting from vascular obstruction and red cell hemolysis of the sickle cell (Ballas 2012). Biochemical abnormalities, including elevation of alkaline phosphatases, total bilirubin, and γ‐glutamyl transpeptidase, typically precede the development of jaundice (Carey 2012). Fatigue and pruritus are the most common symptoms associated with cholestasis (Carey 2012). Acute pain in the right upper quadrant is common in people with SCD and described as right upper quadrant syndrome (Ballas 2012). This syndrome must be separated from the more common symptoms of SCD, i.e., hepatic crisis, hepatic sequestration, autoimmune hepatitis, viral hepatitis, hepatic siderosis, sickle cell intrahepatic cholestasis or sickle cell hepatopathy, cholelithiasis, biliary sludge, choledocholithiasis, acute cholecystitis, and chronic cholecystitis (Ballas 2012). Hepatic sequestration is a component of the right upper quadrant syndrome and it is best diagnosed by a rapid enlargement of the liver with a concurrent drop in hemoglobin concentration. Furthermore, the bilirubin will also be elevated, with a high percentage of direct bilirubin (Ballas 2012).

According to a recent expert panel report, people with acute sickle cell intrahepatic cholestasis show a sudden onset of right upper quadrant pain, severe jaundice due to extreme hyperbilirubinemia (both conjugated and unconjugated) usually without urobilinogenuria, a progressively enlarging and exquisitely tender liver and light‐colored stools (NIH 2014; Yawn 2014). Furthermore, thrombocytopenia, elevated alkaline phosphatase, variable levels of transaminases, coagulopathy with increased prothrombin time, and partial thromboplastin time to values more than twice baseline values in the absence of accelerated hemolysis or obstruction of the extrahepatic biliary system may also be present.

The clinical picture suggests cholestatic jaundice or choledocholithiasis but without evidence of common duct obstruction or cholangitis. Sickle cell intrahepatic cholestasis is an uncommon but potentially fatal complication with a high death rate (Brunetta 2011; Khan 2011). The disease is caused by diffuse sickling within the hepatic sinusoids that ultimately leads to hypoxic hepatic damage and acute hepatic failure (Khan 2011). Liver biopsies of these people show erythrocytosis, erythrophagocytosis, sinusoidal dilatation and hyperplasia in Kupffer cells (Johnson 1985; Omata 1986; Savafi 2006). Furthermore, sickle cell intrahepatic cholestasis is associated with an increased risk of pericardial tamponade (Khurshid 2002), and renal failure (Khan 2011). Older age and underlying hepatic disease have been suggested as poor prognostic factors for sickle cell intrahepatic cholestasis in adults (Costa 2006).

Description of the intervention

Non‐pharmaceutical interventions

1. Simple red blood cell transfusion for increasing oxygen delivery.

2. Exchange transfusion. Red cell exchange or erythrocytapheresis is the most frequently recommended intervention for treating intrahepatic cholestasis in people with SCD (Chitturi 2002; Costa 2006; Danielson 2002; Horn 1987; Karunatilake 2009; O'Callaghan 1995; Sheehy 1980; Tiftik 2004). In 1980, Sheehy and colleagues pioneered the use of this procedure in SCD (Sheehy 1980). This Cochrane Review will use exchange transfusion as the term for this procedure. In exchange transfusion the patient’s red cells are removed and replaced by exogenous normal red cells. The aim is to raise the level of hemoglobin A to between 60% and 70% while lowering the level of hemoglobin S to 30% and reverse bilirubin levels to normal values (Delis 2006; Donghaile 2013). This procedure can be carried out manually or mechanically (Kleinman 1984).

3. Liver transplantation (Gardner 2014).

Pharmaceutical interventions

Several pharmacological therapies have been used to treat people affected by intrahepatic cholestasis in other clinical settings (Angulo 2000; Azzaroli 2011; Carey 2012; Geenes 2009; Muriel 2008). This Cochrane Review will include interventions for treating cholestasis‐associated pruritus: bile acid‐binding resins (i.e., cholestyramine, colestipol); rifampin; opiate antagonists (naltrexone and nalmefene); sertraline; dexamethasone; guar gum; and activated charcoal.

How the intervention might work

Non‐pharmaceutical interventions

1. Simple red blood cell transfusion increasing the hemoglobin and hematocrit levels.

2. Exchange transfusion prevents the removed sickle cells from participating in new vaso‐occlusive events, reduces hemolytic complications, and provides added oxygen carrying capacity while decreasing the blood viscosity (Swerdlow 2006). Red cell exchange also rapidly decreases the rate of hemolysis, which can decrease liver processing of bilirubin, damage to renal tubular cells and the scavenging of nitric oxide by free hemoglobin released from sickle cells (Akinsheye 2010; Donghaile 2013; Kato 2007; Morris 2008).

3. Liver transplantation is a transient therapy approach; however, it does not resolve the fundamental issue.

Pharmaceutical interventions

For treating cholestasis‐associated pruritus, bile acid‐binding resins (i.e., cholestyramine, colestipol), rifampin, opiate antagonists (naltrexone and nalmefene), sertraline, dexamethasone, guar gum and activated charcoal have the ability to bind biliary acids in the gut lumen and block their absorption (Azzaroli 2011; Carey 2012). However, there is potential for these agents to interfere with the absorption of other medications (Carey 2012). Opiate antagonists reduce the increased level of opioidergic tone associated with cholestatic pruritus.

Why it is important to do this review

While exchange transfusion is used for treating intrahepatic cholestasis in people with SCD, there appears to be no specific evidence supporting this medical approach. Exchange transfusion requires packed red blood cell units which have undergone pre‐storage leukoreduction in order to prevent febrile non‐hemolytic reactions and which are screened for sickle cell traits to avoid transfusing red cells containing hemoglobin S (Sarode 2006). Due to a discrepancy of red cell antigens between African‐Americans and Caucasians (majority blood donors), the incidence of alloantibody formation is very high, which makes it difficult to find compatible red cell units, especially for urgent red cell exchange (Sarode 2006). Therefore, this requires a concerted effort between the apheresis unit, the local blood bank, and the central blood supplier (Sarode 2006). Therapeutic apheresis is a relatively safe procedure; however, it is associated with adverse events. These include hypocalcemia due to citrate; increased frequency of bleeding complications and heparin‐induced thrombocytopenia associated with heparin anticoagulation; urticarial reactions to the protein‐containing replacement fluid; depletion coagulopathy and immunoglobulin depletion; catheter‐related trauma; clotting; infection; and bleeding (Kaplan 2012; Lee 2012). Additionally, the benefits and harms of the alternative non‐pharmaceutical intervention, liver transplantation, should be assessed in this clinical setting (Baichi 2005; Emre 2000). This is an update of a previously published Cochrane Review (Martí‐Carvajal 2015 ).

Furthermore, clinical effectiveness and safety of the pharmacological therapies used to treat intrahepatic cholestasis in other clinical settings should be reviewed in people with SCD affected by this hepatic disorder.

Objectives

To assess the benefits and harms of the interventions for treating intrahepatic cholestasis in people with SCD.

Methods

Criteria for considering studies for this review

Types of studies

Randomised controlled trials. 

Types of participants

People with SCD, irrespective of age, gender or setting (e.g. hospital or community) with intrahepatic cholestasis.

Types of interventions

A single or combined treatment regimen (with each treatment classified as non‐pharmaceutical or pharmaceutical, as detailed below) compared to either conventional care or another treatment regimen for intrahepatic cholestasis in people with SCD.

We did not apply any limits with respect to the period of follow up.

Non‐pharmaceutical interventions

  1. Simple red blood cell transfusion

  2. Exchange transfusion

  3. Liver transplantation

Pharmaceutical interventions

  1. For treating cholestasis‐associated pruritus: bile acid‐binding resins (i.e., cholestyramine, colestipol); rifampin; opiate antagonists (naltrexone and nalmefene); sertraline; dexamethasone; guar gum; and activated charcoal.

Types of outcome measures

Primary outcomes

  1. All‐cause mortality

  2. Lack of improvement (as defined by trial authors)

  3. Adverse events

    1. serious adverse events

    2. non‐serious adverse events

We defined serious adverse events according to the International Conference on Harmonisation (ICH) Guidelines (ICH‐GCP 1997), as any event that leads to death, is life‐threatening, requires hospitalisation or prolongation of existing hospitalisation, or results in persistent or significant disability. All other adverse events have been considered as non‐serious.

Secondary outcomes

  1. Quality of life (as measured by the Pediatric Quality of life Inventory (PedsQL™) or Medical Outcomes 36‐Item Short‐Form Health Survey (SF‐36) questionnaire or by any validated scale)

  2. Relief of fatigue (as measured by the PedsQL™ Multidimensional Fatigue Scale or by any validated scale)

  3. Platelet count*

*post hoc change ‐ please refer to the section ‐ Differences between protocol and review.

Search methods for identification of studies

We did not adopt any language or publication restrictions.

Electronic searches

We identified relevant studies from the Cystic Fibrosis and Genetic Disorders Group's Haemoglobinopathies Trials Register using the terms: (sickle cell OR (haemoglobinopathies AND general)) AND liver.

The Haemoglobinopathies Trials Register is compiled from electronic searches of the Cochrane Central Register of Controlled Trials (CENTRAL) (updated each new issue of the Cochrane Library) and weekly searches of MEDLINE. Unpublished work is identified by searching the abstract books of five major conferences: the European Haematology Association conference; the American Society of Hematology conference; the British Society for Haematology Annual Scientific Meeting; the Caribbean Public Health Agency Annual Scientific Meeting (formerly the Caribbean Health Research Council Meeting); and the National Sickle Cell Disease Program Annual Meeting. For full details of all searching activities for the register, please see the relevant section of the Cochrane Cystic Fibrosis and Genetic Disorders Group's website.

Date of last search: 12 April 2017.

We also searched in the following databases:

  1. LILACS (http://lilacs.bvsalud.org) (1982 to 23 May 2017);

  2. Epistemonikos (www.epistemonikos.org) (up to 23 May 2017).

In addition, we searched trial registries via the WHO International Clinical Trials Registry Platform search portal (ICTRP) (http://apps.who.int/trialsearch/Default.aspx) and ClinicalTrials.gov (www.clinicaltrials.gov) (23 May 2017).

Searching other resources

We aimed to check the reference lists of all the trials identified by the above methods. However, we did not identify any randomised controlled trials.

Data collection and analysis

We were unable to identify any randomised controlled trials eligible for inclusion in this review. Therefore, we could not perform the data analyses that we had planned. If, in the future, trials are identified and included in the review, we will adhere to the protocol described below:

Selection of studies

Arturo Martí‐Carvajal (AMC) and Cristina Martí‐Amarista (CMA) will screen the search results for potentially relevant trials and independently assess them for inclusion or exclusion, using a pre‐designed eligibility form based on the inclusion criteria. We will resolve any disagreements through discussion until we reach a consensus.

Data extraction and management

For the future update, one author (AMC) will extract data from the included trials using a spreadsheet data extraction form and one author (CMA) will check the data entered.

We will extract the following data:

  • eligibility criteria of the trials;

  • demographics (age, sex, country);

  • hemoglobin genotype: sickle cell anemia (Hb SS); hemoglobin S combined with hemoglobin C (Hb SC); hemoglobin S associated with ß thalassemia (Sß0 Thal and Sß+ Thal);

  • hepatic biochemistry at time of entry and at end of trial (total, unconjugated and conjugated bilirubin, alkaline phosphatase, alanine aminotransferase, aspartate aminotransferase, gamma‐glutamyltransferase, albumin, prothrombin time);

  • outcome data (all‐cause mortality, lack of improvement, adverse events, quality of life, numbers of jaundice, itching, and being tired, liver biopsy);

  • intervention data: type and regimens.

We will discuss any discrepancies between the review authors to achieve a final consensus.

We aim to pool outcome data from trials based on the following follow‐up periods (zero to one week, over one week to four weeks, over four weeks to 24 weeks and over 24 weeks). If outcome data do not permit such grouping, we shall pool the end‐point data. These different time points are arbitrary and based on clinical judgment.

Assessment of risk of bias in included studies

For the future update, two review authors will independently assess the risk of bias of each included trial using the domain‐based evaluation as described in the Cochrane Handbook for Systematic Reviews of Interventions (Higgins 2011). We will discuss any discrepancies in an aim to achieve consensus.

We will assess the following domains, as per the definitions of each classification below (Higgins 2011).

Generation of allocation sequence (checking for possible selection bias)

We will describe the method used to generate the allocation sequence in each included trial in sufficient detail to allow an assessment of whether it should produce comparable groups.

We will assess the method as:

  • low risk (any truly random process, e.g. random number table, computer random number generator);

  • high risk (any non‐random process, e.g. odd or even date of birth; hospital or clinic record number);

  • unclear (if the trial was described as randomised but the method used for the allocation sequence generation was not described).   

Allocation concealment (checking for possible selection bias)

We will describe the method used to conceal the allocation sequence in each included trial in sufficient detail to determine whether intervention allocation could have been foreseen, in advance of or during recruitment, or changed after assignment.

We will assess the methods as:

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

  • high risk (open random allocation, unsealed or non‐opaque envelopes, alternation, date of birth);

  • unclear (if the trial was described as randomised but the method used to conceal the allocation was not described).

Blinding or masking (checking for possible performance bias)

For each included study we will describe the methods used, if any, to blind trial participants and personnel from knowledge of which intervention a participant received. We will judge trials at low risk of bias if they were blinded, or if we judged that the lack of blinding did not affect the results. We will assess blinding separately for different outcomes or classes of outcomes.

We will assess the methods as:

  • low risk, high risk, or unclear for participants;

  • low risk, high risk, or unclear for personnel;

  • low risk, high risk, or unclear for outcome assessors.

Incomplete outcome data (checking for possible attrition bias through withdrawals, dropouts, protocol deviations)

  • Low risk (any one of the following): no missing outcome data; reasons for missing outcome data unlikely to be related to true outcome (for survival data, censoring unlikely to be introducing bias); missing outcome data balanced in numbers across intervention groups, with similar reasons for missing data across groups; for dichotomous outcome data, the proportion of missing outcomes compared with observed event risk not enough to have a clinically relevant impact on the intervention effect estimate; for continuous outcome data, plausible effect size (difference in means or standardised difference in means) among missing outcomes not enough to have a clinically relevant impact on observed effect size; missing data have been imputed using appropriate methods.

  • High risk (any one of the following): reason for missing outcome data likely to be related to true outcome, with either imbalance in numbers or reasons for missing data across intervention groups; for dichotomous outcome data, the proportion of missing outcomes compared with observed event risk enough to induce clinically relevant bias in intervention effect estimate; for continuous outcome data, plausible effect size (difference in means or standardised difference in means) among missing outcomes enough to induce clinically relevant bias in observed effect size; ‘as‐treated’ analysis done with substantial departure of the intervention received from that assigned at randomisation; potentially inappropriate application of simple imputation.

  • Unclear risk (any one of the following): insufficient reporting of attrition or exclusions to permit judgement of 'low risk' or 'high risk' (e.g. number randomised not stated, no reasons for missing data provided); the study did not address this outcome.

Selective reporting bias (reporting bias due to selective outcome reporting)

We will describe for each included trial how we investigated the possibility of selective outcome reporting bias and what we found.

We will assess the methods as follows.

  • Low risk (any one of the following): the trial protocol is available and all of the trial’s pre‐specified (primary and secondary) outcomes that are of interest in the review have been reported in the pre‐specified way, or the trial protocol is not available but it is clear that the published reports include all expected outcomes, including those that were pre‐specified (convincing text of this nature may be uncommon).

  • High risk (any one of the following): not all of the trial's pre‐specified primary outcomes have been reported; one or more primary outcomes is reported using measurements, analysis methods or subsets of the data (e.g. subscales) that were not pre‐specified; one or more reported primary outcomes were not pre‐specified (unless clear justification for their reporting is provided, such as an unexpected adverse effect); one or more outcomes of interest in the review are reported incompletely so that they cannot be entered in a meta‐analysis; the trial report fails to include results for a key outcome that would be expected to have been reported for such a trial.

  • Unclear: insufficient information to permit judgement of ‘low risk’ or ‘high risk’.

Other bias (bias due to problems not covered elsewhere in the table)

We will describe for each included trial any important concerns we have about other possible sources of bias (baseline imbalance, sponsorship bias, confirmation bias, bias of the presentation data, etc).

  • low risk of bias, the trial appears to be free of other components that could put it at risk of bias;

  • unclear, the trial may or may not be free of other components that could put it at risk of bias;

  • high risk of bias, there are other factors in the trial that could put it at risk of bias, e.g. no sample size calculation made.

Overall risk of bias

We will made explicit judgements about whether trials were at high risk of bias, according to the criteria given in the Cochrane Handbook for Systematic Reviews of Interventions (Higgins 2011). We will assess the likely magnitude and direction of bias, and whether we will consider it likely to impact our findings. 

We will regard trials assessed as having a 'low risk of bias' in all of the individually‐specified domains above as 'trials with an overall low risk of bias'. We will consider trials assessed as having an 'uncertain risk of bias' or a 'high risk of bias' in one or more of the above‐specified individual domains as trials with 'an overall high risk of bias'.

Measures of treatment effect

For future updates, if we are able to include trials, we will perform meta‐analyses according to the recommendations of the Cochrane Collaboration (Higgins 2011). We will use Review Manager 5 to analyse the data (RevMan 2014).

For binary outcomes, such as all‐cause mortality, lack of improvement, and adverse events, we will calculate the risk ratio (RR) with the corresponding 95% confidence intervals (CI).

For continuous outcomes, such as quality of life, and relief of fatigue, the authors will calculate the mean difference (MD) with the corresponding 95% CI. However, if these outcomes are measured using different scales the authors plan to use the standardized mean difference (SMD) with the corresponding 95% CI.

Unit of analysis issues

For future updates, if we are able to include trials, we will use the randomised SCD participant as the unit of analysis.

We do not regard cross‐over trials or cluster randomised trials to be suitable designs for this intervention.

Dealing with missing data

For future updates, if we are able to include trials, we will contact the lead author of each trial in an attempt to obtain the relevant information or missing data (or both). If no further information is available, we will carry out an available case analysis as our main analysis, that is, the denominator for each outcome in each trial will be the number randomised minus the number of participants whose outcomes were known to be missing.

We will assess the percentage of dropouts for each included trial, and for each trial group, and evaluate whether an intention‐to‐treat (ITT) analysis has been performed or could have been performed from the available published information.

Intention‐to‐treat analyses

Regarding the primary outcomes, we will include participants with incomplete or missing data in sensitivity analyses by imputing them according to the following scenarios (Hollis 1999).

  • Poor‐outcome analysis: assuming that dropouts or participants lost from both the experimental and the control arms experienced the outcome, including all randomised participants in the denominator.

  • Good‐outcome analysis: assuming that none of the dropouts or participants lost from the experimental and the control arms experienced the outcome, including all randomised participants in the denominator.

  • Extreme‐case analysis favouring the experimental intervention ('best‐worse' case scenario): none of the dropouts or participants lost from the experimental arm, but all of the dropouts or participants lost from the control arm experienced the outcome, including all randomised participants in the denominator.

  • Extreme‐case analysis favouring the control ('worst‐best' case scenario): all dropouts or participants lost from the experimental arm, but none from the control arm experienced the outcome, including all randomised participants in the denominator.

Assessment of heterogeneity

For future updates, if we are able to include trials, we will visually assess the forest plot for heterogeneity and use the I² statistic and the Q test (P < 0.1) to measure statistical heterogeneity between the trials. The I² statistic describes the percentage of total variation between trials due to heterogeneity rather than sampling error (Higgins 2003). We will consider there to be significant heterogeneity if I² is more than 50% (Higgins 2011).

Assessment of reporting biases

For future updates, if we are able to include trials, if 10 or more trials are available, we will assess publication bias and other biases by the use of a funnel plot (Sterne 2011).

Data synthesis

For future updates, if we are able to include trials, we plan to conduct separate meta‐analyses for the intervention groups (non‐pharmaceutical interventions and pharmaceutical interventions).

If the eligible trials are sufficiently comparable in their clinical characteristics, we will use a random‐effects model and a fixed‐effect model meta‐analysis. If there is discrepancy between the two models (e.g., one giving a significant intervention effect, the other no significant intervention effect) we will report both results; otherwise, we will report only the data using the random‐effects model.

Subgroup analysis and investigation of heterogeneity

If we identify significant heterogeneity in a future update and we are able to include at least 10 trials in the meta‐analysis, we will investigate the possible causes. We will devote further research to identify the possible causes for this heterogeneity, exploring the condition of the individuals.

We anticipate possible clinical heterogeneity in the effect of the intervention and if we find this we plan to conduct the following subgroup analyses if possible:

  • HbSS type versus HbSC type;

  • geographical location of randomised controlled trial;

  • participants' age: less than 18 years old compared to 18 years old and older;

  • type of pharmaceutical intervention.

We will only conduct these subgroup analyses for primary outcomes.

Sensitivity analysis

For any future update, if we include 10 or more trials, we plan to conduct sensitivity analyses including only trials with an 'overall low risk of bias' (Higgins 2011). It is unlikely we will find many trials with an overall low risk of bias, therefore, we plan to choose three core domains: generation of allocation sequence; incomplete outcome data; and selective reporting bias.

Trial sequential analysis

Meta‐analysis of cumulative data may run the risk of random errors ('play of chance') due to sparse data and repetitive analyses of the same data (Brok 2008; Brok 2009; Thorlund 2010; Thorlund 2011; Wetterslev 2008; Wetterslev 2009; Wetterslev 2017). In order to assess the risks of random errors in our cumulative meta‐analyses, we will conduct diversity‐adjusted trial sequential analyses based upon the proportion with the outcome in the control group; an a priori set relative risk reduction of 20%; an alpha of 5%, an beta of 20%; and the squared diversity in the meta‐analysis (Thorlund 2009; Thorlund 2011; CTU 2011). For any future update, we will conduct sensitivity analysis of the trial sequential analysis to estimate the need for further trials.

Summary of findings tables

If, in the future, trials are identified and included in the review, we plan to use the principles of the GRADE system to assess the quality of the body of evidence associated with specific outcomes where possible (all‐cause mortality, lack of improvement, quality of life, and adverse events) (Guyatt 2011a). We will construct a 'Summary of Findings (SoF) table' using the GRADE software (GRADEPro 2008). The GRADE approach appraises the quality of a body of evidence based on the extent to which one can be confident that an estimate of effect or association reflects the item being assessed. The quality of a body of evidence is considered to be: within‐study risk of bias (methodologic quality); the directness of the evidence; heterogeneity of the data; precision of effect estimates; and risk of publication bias (Balshem 2011; Guyatt 2011b; Guyatt 2011c; Guyatt 2011d; Guyatt 2011e; Guyatt 2011f; Guyatt 2011g; Guyatt 2011h; Guyatt 2011i; Guyatt 2012).

Results

Description of studies

Results of the search

In this first update, we identified no potentially relevant references through the initial bibliographical searches on interventions for treating intrahepatic cholestasis in people with SCD.

Risk of bias in included studies

No trials were included.

Effects of interventions

The searches did not identify any randomised controlled trials eligible for inclusion in this Cochrane Review (nor any that were potentially eligible), nor were we able to identify any ongoing trials.

Discussion

Summary of main results

For this first update, we have been unable to identify any randomised controlled trials (RCTs) addressing the benefits and harms of either non‐pharmaceutical (simple red blood cell transfusion, exchange transfusion and liver transplantation) or pharmaceutical interventions (for treating cholestasis‐associated pruritus: bile acid‐binding resins (i.e. cholestyramine, colestipol); rifampin; opiate antagonists (naltrexone and nalmefene); sertraline; dexamethasone; guar gum; and activated charcoal for treating intrahepatic cholestasis in people with sickle cell disease (SCD).

Overall completeness and applicability of evidence

SCD is a major public health problem (WHO 2006; Modell 2008) with an estimated 70% of those affected living in Africa (Tluway 2017), the lack of RCTs to assess the clinical benefits and harms of the interventions for treating intrahepatic cholestasis in people with SCD is perplexing. In 2005, Lottenberg stated "The application of evidence‐based medicine to the management of adults with sickle cell disease is currently primarily driven by clinical expertise and patient preference, as there is a paucity of randomized controlled trial data to guide decision‐making" (Lottenberg 2005). This updated Cochrane Review provides strong evidence in support of Lottenberg's words.

SCD is a vasculopathy (Kassim 2013; Kato 2009). There are several studies reporting the findings of the molecular biology for explaining the endothelial damage in SCD (Caboot 2014; Goodman 2013; Gutsaeva 2014; Kato 2006; Kato 2008; Kato 2009; Kato 2014; Lockwood 2014; Morris 2014; Nishank 2013; Patel 2014; Sun 2013; Thakur 2014; Zhang 2012). They could explain the severe complications of these people and could be used as mechanistic reasoning for supporting RCTs in this condition. Certainly, the scientific uncertainty is undeniable. It is widely known that clinicians make practical decisions, often on the basis of inadequate information. Decisions on treatment should be taken based on the results of RCTs (Alderson 2004; Chalmers 2004).

The rationale for using either non‐pharmaceutical or pharmaceutical treatments for intrahepatic cholestasis in SCD remains unknown. RCTs to answer the research question of this Cochrane Review have not yet been carried out. It is possible that some trials have been conducted, but due to their negative results, they remain unpublished (Easterbrook 1991; Gluud 1998). We can not support or rule out that trials on this subject are unpublished, which is not surprising as was recently highlighhted (Glasziou 2017). This causes publication bias, reducing the possibility of developing valid systematic reviews (Diringer 2003). This is influenced by a number of factors, from the prevalence of the conditions to the resources available to undertake research. Keeping clinical uncertainty hidden does not benefit patients and may increase health‐service costs (Alderson 2000). Conversely, admitting clinical uncertainty helps clarify treatment options and encourages further research (Alderson 2000; Diringer 2003).

We have concluded that intrahepatic cholestasis is a neglected complication of SCD. The paucity of data on clinical benefits and harms of treatments for intrahepatic cholestasis in SCD should stimulate the development of well‐planned RCTs. Recently, a number of recommendations have been suggested in order to increase the value of and to reduce waste in biomedical research (Chalmers 2014; Macleod 2014).

Quality of the evidence

Randomised controlled trials were not identified.

Potential biases in the review process

While performing this systematic review, we also planned to look for 'significance‐chasing biases' (Ioannidis 2010) which include, among others, publication bias, selective outcome reporting bias, selective analysis reporting bias, and fabrication bias (Ioannidis 2010). Publication bias represents a major threat to the validity of systematic reviews, particularly in reviews that include small trials. However, this Cochrane Review contains no trials and as such, no risk of bias could be evaluated. Trials with ‘negative’ results may have remained unpublished as suppression of information on specific outcomes may have occurred (Ioannidis 2010). We have been unable to identify evidence from randomised controlled trials supporting the use of any intervention either non‐pharmaceutical or pharmaceutical for intrahepatic cholestasis in SCD.

The main limitation of this Cochrane Review is the paucity of evidence in people with SCD suffering from intrahepatic cholestasis.

Agreements and disagreements with other studies or reviews

There are no other reviews or studies to compare with this Cochrane Review.