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Antagonistas de los receptores opioides μ para la disfunción intestinal inducida por opiáceos en personas con cáncer y en personas que reciben cuidados paliativos

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Resumen

Antecedentes

La disfunción intestinal inducida por opiáceos (DIIO) se caracteriza por estreñimiento, evacuación incompleta, distensión abdominal y reflujo gástrico. Es uno de los principales eventos adversos (EA) del tratamiento para el dolor en el cáncer y en los cuidados paliativos, y da lugar a una mayor morbilidad y a una reducción en la calidad de vida.

Esta revisión es una actualización parcial de una revisión de 2008, y analiza, como la actualización anterior (2018), solo los ensayos en personas con cáncer y personas que reciben cuidados paliativos.

Objetivos

Evaluar para la DIIO, en personas con cáncer y en personas que reciben cuidados paliativos, la efectividad y la seguridad de los antagonistas de los receptores opioides μ (MOA por sus siglas en inglés) versus diferentes dosis de MOA, intervenciones farmacológicas/no farmacológicas alternativas, placebo o ningún tratamiento.

Métodos de búsqueda

Se realizaron búsquedas en CENTRAL, MEDLINE, Embase, CINAHL y Web of Science (diciembre de 2021), en registros de ensayos clínicos y en sitios web de autoridades sanitarias. Se intentó establecer contacto con fabricantes de MOA para obtener más datos.

Criterios de selección

Ensayos controlados aleatorizados (ECA) que evaluaran la efectividad y la seguridad de los MOA para la DIIO en personas con cáncer y en personas que reciben cuidados paliativos, independientemente del tipo de enfermedad terminal.

Obtención y análisis de los datos

Dos autores de la revisión evaluaron el riesgo de sesgo y extrajeron los datos. Se consideró adecuado combinar los datos de los ensayos si había homogeneidad suficiente entre ellos. Los desenlaces principales fueron la respuesta de laxación, el efecto sobre la analgesia y los EA. La certeza de la evidencia se evaluó mediante GRADE y se crearon tablas de resumen de los hallazgos.

Resultados principales

Se incluyeron diez estudios (dos ensayos nuevos) que asignaron al azar un total de 1343 adultos con cáncer, independientemente del estadio, o en el estadio de cuidados paliativos de cualquier enfermedad. Los MOA fueron la naldemedina y la naloxona orales (solas o en combinación con oxicodona) y la metilnaltrexona subcutánea. Los ensayos compararon los MOA con placebo, los MOA a diferentes dosis o en combinación con otros fármacos. Dos ensayos de naldemedina y tres de naloxona con oxicodona se realizaron en personas con cáncer, independientemente del estadio de la enfermedad. El ensayo sobre la naloxona sola se realizó en personas con cáncer avanzado. Cuatro ensayos sobre la metilnaltrexona se realizaron en cuidados paliativos, donde la mayoría de participantes presentaba cáncer avanzado. Todos los ensayos fueron vulnerables a los sesgos; en la mayoría de los casos no se informó sobre el cegamiento del evaluador de desenlaces.

Naldemedina oral versus placebo

El riesgo (es decir, la probabilidad) de laxaciones espontáneas a medio plazo (en dos semanas) para la naldemedina fue más de tres veces la razón de riesgos (RR) 2,00; intervalo de confianza (IC) del 95%: 1,59 a 2,52; dos ensayos, 418 participantes, I² = 0%. El número necesario a tratar para obtener un desenlace beneficioso adicional (NNTB) fue 3; IC del 95%: 3 a 4; evidencia de certeza moderada. No se informó sobre el riesgo anterior de laxaciones espontáneas ni sobre la evaluación de los cambios intestinales por parte del paciente. Evidencia de certeza muy baja mostró que la naldemedina tuvo poco o ningún efecto sobre los síntomas de abstinencia de los opiáceos. Hubo poca o ninguna diferencia en el riesgo de EA graves (no mortales) (RR 3,34; IC del 95%: 0,85 a 13,15: evidencia de certeza baja). Se informó que hubo más del doble de riesgo de EA (no graves) con la naldemedina (evidencia de certeza moderada).

Dosis bajas de naldemedina oral versus dosis más altas

El riesgo de laxaciones espontáneas fue menor para la dosis más baja (a medio plazo, 0,1 mg versus 0,4 mg: RR 0,69; IC del 95%: 0,53 a 0,89; un ensayo, 111 participantes; evidencia de certeza baja). No se informó sobre el riesgo anterior de laxaciones espontáneas ni sobre la evaluación de los cambios intestinales por parte del paciente. Evidencia de certeza baja mostró poca o ninguna diferencia en cuanto a los síntomas de abstinencia de los opiáceos (0,1 mg versus 0,4 mg; diferencia de medias [DM] ‐0,30; IC del 95%: ‐0,85 a 0,25), y a la aparición de EA graves (0,1 mg versus 0,4 mg; RR 0,25; IC del 95%: 0,03 a 2,17). Evidencia de certeza baja mostró poca o ninguna diferencia en los EA no graves.

Naloxona oral versus placebo

No se ha informado sobre el riesgo de laxaciones espontáneas ni sobre los EA. Poca o ninguna diferencia en la intensidad del dolor (evidencia de certeza muy baja). No se proporcionan los datos completos. El ensayo informó que no se produjeron EA graves.

Naloxona oral + oxicodona versus oxicodona

No se informó sobre el riesgo de laxaciones espontáneas en 24 horas ni a medio plazo. Evidencia de certeza baja mostró que la naloxona con oxicodona redujo el riesgo de síntomas de abstinencia de los opiáceos. Hubo poca o ninguna diferencia en el riesgo de EA graves (no mortales) (RR 0,68; IC del 95%: 0,44 a 1,06; tres ensayos, 362 participantes; I² = 55%; evidencia de certeza muy baja). Hubo poca o ninguna diferencia en el riesgo de EA (evidencia de certeza baja).

Metilnaltrexona subcutánea versus placebo

El riesgo de laxaciones espontáneas en 24 horas con la metilnaltrexona fue cuatro veces mayor que con el placebo (RR 2,97; IC del 95%: 2,13 a 4,13; dos ensayos, 287 participantes, I² = 31%; NNTB 3; IC del 95%: 2 a 3; evidencia de certeza baja). El riesgo de laxaciones espontáneas a medio plazo fue diez veces mayor con la metilnaltrexona (RR 8,15; IC del 95%: 4,76 a 13,95; dos ensayos, 305 participantes, I² = 47%; NNTB 2; IC del 95%: 2 a 2; evidencia de certeza moderada). Evidencia de certeza baja mostró que la metilnaltrexona redujo el riesgo de síntomas de abstinencia de los opiáceos y no aumentó el riesgo de EA graves (RR 0,59; IC del 95%: 0,38 a 0,93; I² = 0%, dos ensayos, 364 participantes). El riesgo de EA fue mayor para la metilnaltrexona (evidencia de certeza baja).

Metilnaltrexona subcutánea a dosis baja versus a dosis más alta

Hubo poca o ninguna diferencia en el riesgo de laxaciones espontáneas a medio plazo (1 mg versus 5 mg o más: RR 2,91; IC del 95%: 0,82 a 10,39; un ensayo, 26 participantes; evidencia de certeza muy baja), o en la evaluación por parte de los pacientes de la mejoría del estado intestinal (RR 0,98; IC del 95%: 0,71 a 1,35; un ensayo, 102 participantes; evidencia de certeza baja). No se informó sobre la evaluación a medio plazo de las laxaciones espontáneas ni de los EA graves. Hubo poca o ninguna diferencia en los síntomas de abstinencia de los opiáceos (DM ‐0,25; IC del 95%: ‐0,84 a 0,34; un ensayo, 102 participantes) o en la aparición de EA (evidencia de certeza baja).

Conclusiones de los autores

Los resultados de esta actualización sobre la naldemedina y la naloxona con oxicodona se han reforzado con dos nuevos ensayos, pero las conclusiones no han cambiado. Evidencia de certeza moderada de la naldemedina oral sobre el riesgo de laxaciones espontáneas y EA no graves indica que la naldemedina podría mejorar la función intestinal a las dos semanas y aumentar el riesgo de EA en personas con cáncer. Hubo evidencia de certeza baja acerca de los EA graves. Evidencia de certeza moderada de la metilnaltrexona sobre las laxaciones espontáneas a las dos semanas sugiere que la metilnaltrexona subcutánea podría mejorar la función intestinal en las personas que reciben cuidados paliativos, pero la certeza de la evidencia sobre los EA fue baja. Se necesitan más ensayos, más evaluación de los EA, de los desenlaces que los pacientes consideran importantes y en niños.

PICOs

Population
Intervention
Comparison
Outcome

The PICO model is widely used and taught in evidence-based health care as a strategy for formulating questions and search strategies and for characterizing clinical studies or meta-analyses. PICO stands for four different potential components of a clinical question: Patient, Population or Problem; Intervention; Comparison; Outcome.

See more on using PICO in the Cochrane Handbook.

Resumen en términos sencillos

Antagonistas de los receptores opioides mu para la disfunción intestinal por los opiáceos en personas con cáncer y personas que reciben cuidados paliativos

Antecedentes

Los opiáceos (medicamentos similares a la morfina) se utilizan para tratar el dolor intenso, pero pueden provocar disfunciones intestinales, como estreñimiento, evacuación incompleta, gases y aumento del reflujo del contenido del estómago hacia el esófago. Esto se debe a que los receptores de los opiáceos se encuentran en el intestino. La disfunción intestinal inducida por los opiáceos podría ser tan grave que las personas deciden limitar el alivio del dolor para mejorar la función intestinal. La disfunción intestinal inducida por los opiáceos es frecuente en las personas con cáncer y en las que reciben cuidados paliativos (cuando la cura ya no es posible). Los laxantes suelen ser el tratamiento de primera elección para la disfunción intestinal inducida por los opiáceos. Estos medicamentos no siempre funcionan. Los antagonistas de los receptores opioides mu son medicamentos específicos para la disfunción intestinal inducida por los opiáceos que se han desarrollado para ayudar a reducir el efecto de los opiáceos en el intestino. Sin embargo, un posible efecto secundario de este tratamiento es la reducción del alivio del dolor.

Características de los ensayos

El objetivo de esta revisión actualizada fue determinar lo que se conoce acerca de la efectividad y la seguridad de los antagonistas de los receptores opioides mu (MOA por sus siglas en inglés) para el tratamiento de la disfunción intestinal inducida por los opiáceos en personas con cáncer o que reciben cuidados paliativos. Solo se incluyeron ensayos controlados aleatorizados, ya que brindan la evidencia más fiable. Los ensayos controlados aleatorizados son un tipo de estudio en el que las personas se reparten al azar en grupos para evaluar intervenciones, tratamientos o medicamentos. Significa que una persona tiene las mismas posibilidades de recibir cada intervención, tratamiento o medicamento.

Se encontraron ensayos que evaluaron los antagonistas de los receptores opioides mu naldemedina, metilnaltrexona y naloxona. Los grupos de comparación del ensayo podrían ser un placebo (una sustancia sin efecto activo conocido), la atención habitual, otra dosis del antagonista de los receptores opioides mu, el medicamento combinado con otros medicamentos u otro tratamiento como un antagonista de los receptores opioides mu diferente.

Resultados clave

La búsqueda hasta el 20 de diciembre de 2021 encontró diez ensayos con 1343 adultos. Los antagonistas de los receptores opioides mu evaluados en personas con cáncer fueron naldemedina y naloxona orales tomadas en combinación con un tratamiento con opiáceos (para el dolor). El otro antagonistas de los receptores opioides mu evaluado en los ensayos fue la metilnaltrexona. Se administró mediante inyección y se evaluó en cuidados paliativos, donde la mayoría de los participantes presentaban cáncer avanzado.

La naldemedina o la metilnaltrexona se compararon con un placebo. La naloxona se comparó con un placebo o con un tratamiento con opiáceos solamente.

La confianza general expresada como la certeza que se tiene en las pruebas es muy baja a moderada (de muy incierta a algo segura). Hubo problemas con el diseño de los estudios, como la información insuficiente acerca de los métodos del ensayo.

Movimientos intestinales

Durante dos semanas de tratamiento con naldemedina o metilnaltrexona, es probable que los movimientos intestinales aumenten (evidencia moderada/algo segura); los ensayos no midieron los efectos de la naloxona durante dos semanas. Hubo una confianza baja (evidencia incierta) en que los pacientes consideraron que la naloxona tomada junto con un tratamiento con opiáceos y la metilnaltrexona mejoraron sus síntomas de estreñimiento. Los ensayos de naldemedina no midieron la evaluación de los pacientes de una mejoría de los síntomas de estreñimiento.

Alivio del dolor

Hubo una confianza baja en las pruebas de que la naloxona en combinación con un opiáceo o la metilnaltrexona no produjeron efecto en el tratamiento del alivio del dolor. Hubo una confianza baja (incierta) en las pruebas de que la naldemedina no modificó el alivio del dolor en el tratamiento.

Riesgo de efectos secundarios graves (p. ej., hospitalización, potencialmente mortales o mortales) y otros efectos secundarios

Hubo una confianza baja (incierta) en que la naldemedina o la metilnaltrexona no causaron un aumento del riesgo de efectos secundarios graves. Hubo confianza baja en las pruebas de que la naloxona en combinación con un opiáceo no aumentó el riesgo de efectos secundarios graves (reacción adversa).

La naldemedina probablemente no aumentó el riesgo de otros efectos secundarios no graves (certeza moderada/evidencia algo segura). Hubo poca confianza en las pruebas de que la naloxona tomada con el tratamiento con opiáceos no causó un aumento del riesgo de un efecto secundario. Hubo confianza baja en las pruebas de que la metilnaltrexona no aumentó el riesgo de un efecto secundario.

Conclusión

Hubo pruebas de certeza moderada de que la naldemedina tomada por vía oral mejoró la función intestinal durante dos semanas en los adultos con cáncer y disfunción intestinal inducida por los opiáceos, pero aumentó el riesgo de efectos secundarios; también de que la metilnaltrexona administrada por inyección mejoró la función intestinal durante dos semanas en personas que recibían cuidados paliativos. Los resultados de esta revisión se deben interpretar con precaución, ya que no se obtuvieron a partir de pruebas de certeza alta. Las evaluaciones de los desenlaces fueron limitadas, en concreto, no todos los ensayos midieron la evaluación sobre la mejoría de los movimientos intestinales por parte de los pacientes. No se identificaron estudios en niños.

Authors' conclusions

Implications for practice

For people with cancer and people receiving palliative care with opioid‐induced bowel dysfunction

In people with cancer who have opioid‐induced bowel dysfunction (OIBD), despite laxative use, we found moderate certainty in the evidence that the mu‐opioid antagonist (MOA), naldemedine, taken orally may improve bowel function within two weeks of the start of administration. We found very low certainty in the evidence whether naldemedine has little to no increase in risk of increasing symptoms of opioid withdrawal. We found low‐certainty evidence that naldemedine has little to no increase in chances of a serious adverse event. We found moderate‐certainty evidence that naldemedine increases the chances of experiencing a non‐serious adverse event. The most common non‐serious adverse event is diarrhoea. Patient assessment of improvement in bowel status was not reported.

Trials on the effect of naloxone alone or in combination with oxycodone in treating OIBD in people with cancer did not measure bowel function within two weeks of the start of administration. For naloxone in combination with oxycodone we found low‐certainty evidence that it has no impact on symptoms of opioid withdrawal and adverse events, and very low‐certainty evidence that it has no effect on risk of serious adverse events (SAEs).

We found moderate‐certainty evidence in palliative care that when conventional laxatives have failed that the MOA, methylnaltrexone, administered subcutaneously, can be successful within two weeks in improving bowel function. We found low‐certainty evidence that methylnaltrexone improves peoples assessment of their bowel status, improves within 24 hours bowel function, and that it has little to no effect on symptoms of opioid withdrawal. There is low‐certainty evidence that it does not increase the chances of SAEs and that it has little to no effect on adverse events.

We found no studies on children, and no head‐to‐head trials of MOAs (two MOAs compared with each other).

For clinicians

In this update, our overall conclusions have not changed. For people with cancer, there is moderate‐certainty evidence that oral naldemedine may be effective within two weeks of administration in inducing laxation where conventional laxatives have failed. Patient assessment of change in bowel status was not reported in the included trials. There is low‐certainty evidence that naldemedine has little to no impact on symptoms of opioid withdrawal. There were in one of the two trials that assessed naldemedine five serious adverse events in participants in the naldemedine arm, and no serious adverse events in participants taking placebo. It is not clear if any of the events were related to naldemedine. We judged this as low‐certainty evidence on whether this drug increases the risk of serious adverse events. There was low‐certainty evidence that naldemedine did increases the chances of experiencing another (non‐serious) adverse event; commonly this was diarrhoea.

In palliative care where conventional laxatives have failed, there is low‐certainty evidence that methylnaltrexone is effective in the short term (within 24 hours). Over two weeks, there is moderate‐certainty evidence that methylnaltrexone is effective in inducing laxation for a proportion of people in palliative care with OIBD There is low‐certainty evidence that methylnaltrexone improves peoples assessment of their bowel status. There is low‐certainty evidence that methylnaltrexone has little to no impact on symptoms of opioid withdrawal. Methylnaltrexone may be associated with an increase in certain adverse events, such as abdominal pain and flatulence but this evidence is of low certainty. There is low‐certainty evidence to suggest that this medication has little to no increase in the risk of serious adverse events.

Trials on naloxone alone or in combination with oxycodone in treating OIBD in people with cancer did not measure laxation response within two weeks of drug administration. For naloxone in combination with oxycodone there is low‐certainty evidence to support the suggestion that it has little to no impact on analgesia or in the risk of adverse events. There is very low‐certainty evidence that naloxone in combination with oxycodone has little to no impact on the risk of SAEs.

These treatments were tested in studies that excluded patients in situations that may affect efficacy by compounding constipation such as any disease processes suggestive of abnormalities of the gastrointestinal tract, and chemotherapy. All these treatments are unlikely to be effective in all people and not all outcomes have been fully evaluated, for example, treatment satisfaction and preference. We found no studies on children. There have been no head‐to‐head trials, so it is difficult to compare their impact on OIBD.

For policy makers

In adults in palliative care, when conventional laxatives have failed, subcutaneous methylnaltrexone at two weeks, and in people with cancer oral naldemedine at two weeks may be successful in improving bowel function. In adults with cancer and those receiving palliative care, laxatives are first‐line drug therapy. When conventional laxatives have failed, subcutaneous methylnaltrexone is a second‐line therapy if an immediate response is required. Oral naldemedine is a second‐line therapy if an immediate laxation is not essential.

For funders of the intervention

There is sufficient evidence in palliative care for adults that when conventional laxatives have failed subcutaneous methylnaltrexone may improve bowel function within two weeks and low‐certainty evidence it may improve function within 24 hours. There is sufficient evidence that in adults with cancer oral naldemedine may improve bowel function within two weeks of start of administration. Evidence on naldemedine impact on bowel function is not reported. We would encourage funders to consider, when conventional laxatives have failed, subcutaneous methylnaltrexone as a second‐line therapy if an immediate response is required. Oral naldemedine is a second‐line therapy if an immediate laxation is not essential.

Implications for research

We found four trials that were ongoing, and six awaiting further detail on whether they fulfilled our eligibility criteria. This includes evaluation of naloxegol. Therefore, some of the suggestions listed in this section may need to be modified once the results of these trials are published. Two ongoing trials, which were excluded based on our current inclusion criteria of treatment for people with OIBD, are evaluating whether naldemedine alone or as an adjunct may prevent OIBD starting (jRCTs031200397Ozaki 2020). This suggests any future update of this review may want to also consider use of MOAs as a preventative treatment in these patient groups.

General

Rigorous randomised controlled trials (RCTs) measuring standardised and clinically‐ and participant‐relevant outcomes are needed to establish the effectiveness and safety of MOAs. Head‐to‐head comparisons should be considered. Trials should be reported according to the CONSORT statement and its extensions such as for cross‐over trials (Schulz 2010).

Design

Attrition rates in the included trials and the relatively small numbers of eligible participants in any one palliative care treatment unit suggest that trials should involve participants recruited from multiple centres.

Measurement (endpoints)

There is a need to include multiple measures in addition to laxation response, these include analgesia effect, pain intensity, tolerability, quality of life, participant preference, and costs.

Summary of findings

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Summary of findings 1. Naldemedine compared to placebo for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care

Naldemedine compared to placebo for opioid‐induced bowel dysfunction for people with cancer 

Patient or population: people with cancer irrespective of whether receiving palliative care and with opioid‐induced bowel dysfunction

Settings: not stated

Intervention: naldemedine

Comparison: placebo

Outcomes

Illustrative comparative risks* (95% CI)

Relative effect
(95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Placebo

Naldemedine

Laxation response: risk of spontaneous rescue‐free bowel movementsain the short termb

Not reported

Laxation response: risk of spontaneous rescue‐free bowel movementsain the medium termc

355 per 1000 

718 per 1000

RR 2.00 (1.59 to 2.52) NNTB 3 (3 to 4)

418 (2 studies)

⊕⊕⊕⊝

Moderated

 

 

Laxation response: patient assessment of change in bowel status at the end of trial

Not reported

Symptoms of opioid withdrawalein the

medium termc

Mean change in opioid withdrawal was 0.0

Mean change in opioid withdrawal was 0.1 lower 0.1 mg; 0.3 higher 0.2 mg, 0.2 higher 0.4 mg

Naldemedine 0.1 mg: MD ‐0.10 (‐0.56 to 0.36); naldemedine  0.2 mg: MD 0.30 (‐0.21 to 0.81); naldemedine  0.4 mg: MD 0.20 (‐0.36 to 0.76)d

112 in comparison with naldemedine 0.1 mg and 0.4 mg, 114 in comparison with 0.2mg (1 study)

⊕⊝⊝⊝
Very lowf,g

 

Serious adverse eventsh

13 per 1000

41 per 1000

RR 3.34 (0.85 to 13.15)

418 (2 studies)

⊕⊕⊝⊝
Lowd,i

 

Adverse events

355 per 1000

613 per 1000

RR 1.49 (1.19 to 1.87)

418 (2 studies)

⊕⊕⊕⊝

Moderated

 

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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).

RR: risk ratio; NNTB: number needed to treat for an additional beneficial outcome; MD: mean difference

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Defined in both trials as having 3 or more laxations (not induced by rescue medication) a week/who had an increase of one of more laxations (not induced by rescue medication) a week from baseline

b Within first 24 hours

c Over two weeks

d Downgraded by one level for serious study limitations because of high risk of attrition bias in one study

e Measured by the Clinical Opioid Withdrawal Scale. Lower scores indicate symptoms of lower severity. Score of 5‐12 mild, 13‐24 moderate, 25‐36 moderately severe, more than 36 severe withdrawal. Maximum score 48.
f Downgraded by two levels for very serious study limitations because all of the data were derived from only one study with a high risk of attrition bias

g Downgraded by one level for serious imprecision as data were derived from fewer than 400 participants

h Serious non‐fatal events were reported, definition of what fits this criteria was not provided

i Downgraded by one level for serious imprecision due to wide confidence intervals

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Summary of findings 2. Low dose naldemedine compared to higher doses for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care

Low dose naldemedine compared to higher‐dose for opioid‐induced bowel dysfunction for people with cancer 

Patient or population: people with cancer irrespective of whether they are receiving palliative care and with opioid‐induced bowel dysfunction

Setting: not stated

Intervention: Naldemedine 0.1 mg daily

Comparison: Naldemedine 0.4 mg daily

Outcomes

Illustrative comparative risks* (95% CI)

Relative effect
(95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Higher dose

0.4 mg daily

Lower dose

0.1 mg daily

Laxation response: risk of spontaneous rescue‐free bowel movements in the short terma

Not reported

Laxation response: risk of spontaneous rescue‐free bowel movements in the medium termb,c

821 per 1000

564 per 1000

RR 0.69 (0.53 to 0.89)

111 (1 study)

⊕⊕⊝⊝

Lowd,e

 

Laxation response: patient assessment of change bowel status at end of trial

Not reported

Symptoms of opioid withdrawalfin the medium termb

 

Mean change in opioid withdrawal

0.2

Mean change in opioid withdrawal ‐0.3 lower

MD 

‐0.30 [‐0.85, 0.25]

112 (1 study)

 

⊕⊕⊝⊝

Lowd,e

 

Serious adverse eventsg

0.7 per 1000

0.2 per 1000

RR 0.25 (0.03, 2.17)

112 (1 study)

⊕⊕⊝⊝

Lowd.e

 

Adverse events

786 per 1000

 

660 per 1000

RR 0.84 (0.67,1.06)

112 (1 study)

⊕⊕⊝⊝

Lowd,e

 

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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; RR: risk ratio; ; MD: mean difference

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Within first 24 hours following intervention and comparison treatment

b Defined in study as having 3 or more laxations (not induced by rescue medication) a week/who had an increase of one of more laxations (not induced by reduce medication) a week from baseline

c Measured over two weeks
d Downgraded by one level for serious study limitations due to unclear risk of bias (reporting bias)

e Downgraded by one level for serious imprecision (fewer than 400 participants for continuous data or fewer than 300 events for dichotomous data).

fMeasured by the Clinical Opioid Withdrawal Scale. Lower scores indicate symptoms of lower severity. Score of 5‐12 mild, 13‐24 moderate, 25‐36 moderately severe, more than 36 severe withdrawal. Maximum score 48.

g Serious non‐fatal events were analysed, no further definition by study authors

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Summary of findings 3. Naloxone compared with placebo for opioid‐induced bowel dysfunction in people with cancer and receiving palliative care

Naloxone compared with placebo for people with cancer and receiving palliative care with opioid‐induced bowel dysfunction

Patient or population: people with cancer and receiving palliative care with opioid‐induced bowel dysfunction

Settings: community

Intervention: naloxone

Comparison: placebo

Outcomes

Illustrative comparative risks*

Relative effect (95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Placebo

Naloxone

Laxation response: risk of spontaneous rescue‐free bowel movements in the short terma

 

 

Not reported

Laxation response: risk of spontaneous rescue‐free bowel movements in the medium termb

 

 

Not reported

Laxation response: patient assessment of change in bowel status at the end of trial

Not reported

Symptoms of opioid withdrawal in the medium term

17 (1 study) 

Full data not provided 

Serious adverse events

17 (1 study)

⊕⊝⊝⊝

Very lowc,d

No serious adverse events were reported

Adverse events

Not reported

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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).

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Within first 24 hours

b Between 1 and 14 days

Downgraded by one level for serious study limitations: unclear risk of bias (reporting bias) 

Downgraded by two levels for very serious imprecision as sparse data (17 participants)

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Summary of findings 4. Naloxone + oxycodone prolonged release tablets compared with oxycodone prolonged‐released tablets for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care

Naloxone + oxycodone prolonged release tablets compared with oxycodone prolonged‐released tablets for people with cancer and opioid‐induced bowel dysfunction

Patient or population: people with cancer irrespective of whether they were receiving palliative care opioid‐induced bowel dysfunction

Settings: community

Intervention: naloxone + oxycodone prolonged‐release tablets (OXN PR)

Comparison: oxycodone prolonged‐released tablets (OXY PR)

Outcomes

Illustrative comparative risks* (95% CI)

Relative effect (95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Oxycodone (OXY PR)

Oxycodone + naloxone (OXN PR)

Laxation response: risk of spontaneous rescue‐free bowel movements in the short terma

 

 

 

Not reported

Laxation response: risk of spontaneous rescue‐free bowel movements in the medium termb

Not reported

Laxation response: Patient assessment of change in bowel statuscat the end of trial

data not provided

data not provided

Study 1: Mean change ‐ 11.14 (‐19.03, ‐3.24)

Study 2: Little to no change p value = 0.264

212 (2 studies)

⊕⊕⊝⊝

Lowd,e 

Full data not provided in either study

Symptoms of opioid withdrawalfin the medium termb

Mean 7.27

Mean 0.63 lower

MD ‐0.63 (‐2.44, 1.18)

133 (1 study)

⊕⊕⊝⊝

Lowd,e

Serious adverse eventsg

208 per 1000

141 per 1000

RR 0.68 (0.44 to 1.06)

362 (3 studies)

⊕⊝⊝⊝

Very lowd,e,h

Adverse events

584 per 1000

592 per 1000

RR 1.01 (0.87 to 1.18)

362 (3 studies)

⊕⊕⊝⊝

Lowd,e

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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; RR: risk ratio; ; MD: mean difference

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Within first 24 hours

b Between 1 and 14 days

c Measured in one study using 3‐item Bowel Function Index, where lower scores indicate better bowel function, and scores above 28.8 indicate constipation. Scores range from 0 to 100. In the other study change in bowel habits was measured using a 3‐point Likert Scale (worsened, no change, improved)

d Downgraded by one level because of serious study limitations (unclear risk of reporting bias)
e Downgraded by one level because of serious imprecision (data from fewer than 400 participants)

f Measured using the 16‐item Modified Subjective Opiate Withdrawal Scale. Lower scores indicate symptoms of lower severity. Range 0 to 64. Further scoring details not reported

g Not defined by trial authors

Downgraded by one level because of serious unexplained inconsistency (substantial heterogeneity I2 = 55%)

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Summary of findings 5. Methylnaltrexone compared to placebo for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer

Methylnaltrexone compared to placebo for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer

Patient or population: people receiving palliative care irrespective of whether they had cancer with opioid‐induced bowel dysfunction

Setting: hospital and community

Intervention: methylnaltrexone

Comparison: placebo

Outcomes

Anticipated absolute effects* (95% CI)

Relative effect
(95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Risk with placebo

Risk with

methylnaltrexone

Laxation response: risk of spontaneous rescue‐free bowel movementsain the short termb

236 per 1000

701 per 1000 (625 to 770)

RR 2.97 (2.13 to 4.13) NNTB 3 (2 to 3)

287 (2 studies)

⊕⊕⊝⊝

Lowc,d

 

Laxation response: risk of spontaneous rescue‐free bowel movementsain the medium terme

85 per 1000

671 per 1000
(590 to 745)

RR 8.15 (4.76 to 13.95) NNTB 2 (2 to 2)

305
(2 studies)

⊕⊕⊕⊝

Moderatec,f

 

Laxation response: patient assessment of change in bowel statusgat the end of trial

252 per 1000

567 per 1000

(488 to 644)

RR 2.32 (1.64 to 3.27)*

287 (2 studies)

⊕⊕⊝⊝

Lowc,d

Proportion reporting improvement

Symptoms of opioid withdrawalhin the medium term

Mean 8.1

Mean 0.2lower

MD ‐0.20 (‐0.80 to 0.40)

133 (1 study)

⊕⊕⊝⊝

Lowc,d

 

 

Serious adverse eventsi

238 per 1000

142 per 1000
(88 to 219)

RR 0.59 (0.38 to 0.93)

364
(2 studies)

⊕⊕⊝⊝

Lowc,d

 

Adverse events

700 per 1000

797 per 1000
(745 to 869)

RR 1.17

(CI 1.05 to 1.30)

518
(3 studies)

⊕⊕⊝⊝

Lowc,j

Heterogeneity was substantial (74%). We did not undertake a sensitivity analyses as none of our predefined criteria for undertaking one were matched.

*The risk in the intervention group (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; MD: mean difference; RR: risk ratio; NNTB: number needed to treat for an additional beneficial outcome

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate: the true effect is likely to be close to the estimate of the effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited: the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate: the true effect is likely to be substantially different from the estimate of effect.

a Measured by self‐report or clinician report

b Within first 24 hours following intervention and comparison treatment

cDowngraded once for serious study limitations because of unclear risk of reporting bias

dDowngraded once for serious imprecision (data fewer than 400 participants)

eBetween 1 and 14 days

fAs the effect size was large we did not downgrade for imprecision

gMeasured in both studies using the Global Clinical Impression of Change, a scale ranging from 1 to 7, with higher scores indicating better bowel function

hMeasured using the modified Himmelsbach Opioid Withdrawal Scale. Lower scores indicate symptoms of lower severity. Total scores range from 7 to 28.
Not defined by trial authors

jDowngraded once for serious inconsistency because of substantial heterogeneity across trials

*In one trial with 2 comparisons with the same control arm, we combined the intervention groups to form a single pairwise comparison

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Summary of findings 6. Methylnaltrexone lower dose compared to higher dose for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer

Methylnaltrexone 1 mg compared to methylnaltrexone 5 mg or greater for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer

Patient or population: people receiving palliative care irrespective of whether they had cancer with opioid‐induced bowel dysfunction

Setting: hospital and community

Intervention 1: lower‐dose methylnaltrexone (study 1: 3 doses, 1 week, 1 mg; study 2: 1 dose, 0.15 mg/kg)

Intervention 2: higher‐dose methylnaltrexone (study 1: 3 doses, 1 week, 5‐20 mg; study 2: 1 dose, 0.30 mg/kg)

Outcomes

Illustrative comparative risks* (95% CI)

Relative effect
(95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Higher dose (5 mg)?

Lower dose (1 mg)?

Laxation response: risk of spontaneous rescue‐free bowel movementsain the short termb

Study 1: 609 per 1000

Study 2: 639 per 1000

Study 1: 499 per 1000 (250 to 100)

Study 2: 681 per 1000 (515 to 904)

Study 1: RR 0.21 (0.03 to 1.41)

Study 2: 

RR 1.06 (0.77 to 1.46)

135 (2 studies) Study 1: n = 33

Study 2: n = 102

⊕⊕⊝⊝

Lowc,d

Study data not combined as methylnaltrexone dosing differed substantially per study.

Laxation response: risk of spontaneous rescue‐free bowel movementsa,in the medium terme

647 per 1000

222per 1000 

 RR 2.91 (0.82 to 10.39)

 

26 (1 study)

⊕⊝⊝⊝

Very lowc,f

 

Laxation response: patient assessment of change in bowel statusgat the end of trial

58 per 100

60 per 1000

RR 0.98 (0.71 to 1.35)

102 (1 study)

⊕⊕⊝⊝

Lowc,d

 

Symptoms of opioid withdrawal in the medium term

0.25

mean 0.25 lower 

MD ‐0.25 (‐0.84 to 0.34)

102 (1 study)

⊕⊕⊝⊝

Lowc,d

Data not combined as methylnaltrexone dosing differed.

Serious adverse events

In one trial, 15 serious adverse events occurred during the randomised trial phase but it does not report what arm the events occurred in. 

Adverse events

Study 1: 1000 per 1000

Study 2: 800 per 1000

Study 1: 1000 per 1000 (1000 to 1000)

Study 2: 723 per 1000

(580 to 902)

Study 1: RR 1.00 (1.00 to 1.00)

Study 2: RR 0.90 (0.73 to 1.13)

135 (2 studies)

Study 1: n = 33

Study 2: n = 102

⊕⊕⊝⊝

Lowc,d

 

 

Study data not combined as methylnaltrexone dosing differed substantially per study

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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; MD: mean difference; RR: risk ratio.

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Measured by clinician or self‐report

b Within first 24 hours following intervention and comparison treatment

c Downgraded by one level for serious study limitations: unclear risk of bias (reporting bias)

d Downgraded by one level for serious imprecision as fewer than 400 participants.

eBetween 1 and 14 days

f Downgraded by two levels for very serious imprecision as sparse data 26 participants and wide confidence intervals

Background

This is an update of the review first published in 2008 (McNicol 2008), and last updated in 2018 (Candy 2018). It is a partial update of the review published in 2008 entitled Mu‐opioid antagonists for opioid‐induced bowl dysfunction (McNicol 2008). Since publication in 2008, there has been an increase in the number of trials on mu‐opioid antagonists (a drug designed to neutralise the effect of opioids on bowel function), and this current review and its last update critiques evidence only for people with cancer and people receiving palliative care.

Description of the condition

Opioids, such as morphine sulphate, oxycodone, and fentanyl, are potent analgesics (medicines to relieve pain). They are recommended in clinical guidelines by the World Health Organization (WHO) including for the management of moderate‐to‐severe pain from cancer and other populations such as people needing palliative care (WHO 2016). They are widely used, although globally there is wide variation suggesting an under‐utilisation of opioids for pain management in some locations (Manjiani 2014).

However, opioids are associated with adverse events. The most common and disabling of these is bowel dysfunction, which can be severe enough for a person to limit their opioid use (Cook 2008). Opioids, regardless of the method of administration (oral, parenteral, transdermal), interfere with gastrointestinal propulsive motility (Leppert 2010). Opioids increase absorption of fluids from the intestine and decrease epithelial secretion. They delay gastric emptying and decrease peristalsis in the gut.

Opioid‐induced bowel dysfunction (OIBD) has been described as quote: "A change when initiating opioid therapy from baseline bowel habits that is characterised by any of the following: reduced bowel movement frequency (conventionally less than 3 per week), development or worsening of straining to pass bowel movements, a sense of incomplete rectal evacuation, or harder stool consistency" (Kumar 2012). It may even lead to stool impaction (Camilleri 2014). In addition to constipation, OIBD describes a constellation of symptoms including bloating, abdominal distention, gastric reflux, abdominal cramping, dry mouth, epigastric fullness, nausea, and vomiting (Leppert 2015Pappagallo 2001). It can cause psychological distress and agitation in terminally ill people. OIBD increases health service use, sometimes necessitates hospitalisation, and it can dramatically reduce an already compromised quality of life. It may lead to people under‐treating their pain (Pizzi 2012); however, since the dose that produces constipation may only be 25% of that required for adequate analgesia, dose reduction is not an appropriate option for management of OIBD (Ketwaroo 2013).

In people with cancer, hospice populations and people with advanced disease, the estimated incidence of OIBD is high, from 60% to 90% (Glare 2006Panchal 2007Sykes 1998). Although these estimates are relatively old, there is no evidence to suggest that this is no longer the case. Moreover, surveys have found that large proportion of people skip, decrease or discontinue opioid use because of bowel dysfunction, thereby preferring pain in preference to constipation (Gupta 2015Cook 2008LoCasale 2016).

Description of the intervention

The recommended and commonly prescribed preventive and management treatment of OIBD in palliative care and advanced disease is the use of a laxative stimulant and a stool softener, in addition to general measures such as increased food, fibre‐rich diet, fluid intake, physical activity, and privacy during defecation (NICE 2016Larkin 2018Sera 2018). These measures are not always effective; in people taking opioids, it is estimated that over 80% of people remain constipated despite regular use of laxatives (Coyne 2014Diego 2011). This inadequate response can be defined as having at least one opioid‐induced constipation symptom (incomplete bowel movement, hard stools, straining or false alarms) of moderate severity, while taking at least one type of laxative over four days within the past two weeks.

Mu‐opioid antagonists (MOAs), such as methylnaltrexone, naloxone, and naloxegol, are designed specifically to target the pathophysiology of OIBD by 'neutralising' the constipating effect of the opioid. Methylnaltrexone is licensed for the treatment of opioid‐induced constipation in palliative care in more than 50 countries (Bader 2013). In clinical guidelines, where methylnaltrexone or other MOAs are considered, it is described to act as an augmentation to laxatives or as an alternative when laxatives fail (European Association of Palliative Care, Caraceni 2012; European Society of Medical Oncology (ESMO), Larkin 2018), and should be used only under advice from a specialist palliative care clinician (Scottish Palliative Care Guidelines 2014). The National Institute for Health and Care Excellence (NICE) recommends naldemedine (NICE 2020) and naloxegol (NICE 2015) for treating OIBD in adults who have had laxative treatment. This is based on both evidence on effect and cost. NICE does not recommend methylnaltrexone because no evidence submission was received from the manufacturer of the technology (NICE 2017).

How the intervention might work

Opioids mediate their gastrointestinal and analgesic effects through the same subclasses of opioid receptors in the human body: mu, kappa, and delta. How each receptor type is involved in OIBD is not fully understood (Neefjes 2014). The peripheral opioid effect on mu‐opioid receptors in the gut wall may play a main role in OIBD (Leppert 2010). Co‐ordination of motility is disrupted by activation of the mu‐opioid receptors that inhibit excitatory and inhibitory neural pathways within the enteric nervous system.

One approach for dissociation of the analgesic effect of opioids is to separate the opioid's central activity from its peripheral activity (Wang 2013). This may be achieved with a peripherally acting opioid receptor antagonist with limited ability to cross the blood‐brain barrier and which therefore does not interfere with analgesia (Brown 1985). Alternatively, this can be achieved by use of a preparation that undergoes extensive 'first‐pass' metabolism by the liver and so does not enter the systemic circulation.

There are several MOAs in use. Naloxone is commercially available; it is centrally acting but has a narrow therapeutic effect with certain doses reversing desirable analgesia (Camilleri 2011). It undergoes extensive first‐pass metabolism and in the correct dosage it does not reverse the analgesic effect of opioids. It is administered orally. The development of a prolonged‐release preparation of naloxone to allow as much cover of the small and large intestine as possible when used with oxycodone has led to further studies of the compound (Camilleri 2011). There are several other preparations that do not cross the blood‐brain barrier and these include alvimopan, methylnaltrexone, naloxegol, and naldemedine. Alvimopan has a high affinity for peripheral opioid receptors. It is only recommended for short‐term use, such as post‐surgery, because of the possibility of myocardial events (Merck 2015). It is contraindicated in people with advanced disease (Leppert 2015). Methylnaltrexone is less lipid soluble than naloxone and, therefore, less likely to cross the blood‐brain barrier. It is only currently available in subcutaneous formulation. Naloxegol, which is administered orally, has a polyethylene glycol moiety that limits its capacity to cross the blood‐brain barrier (Pritchard 2015). Naldemedine is administered orally, and it is a derivative of naloxone, it has a large polar surface that reduces its ability to access the central nervous system (FDA 2017).

Why it is important to do this review

There are reviews of MOAs for OIBD across different populations (e.g. Nee 2018; Ford 2013). However, it is important to evaluate their effectiveness and safety specifically in cancer and in palliative care populations (Bader 2012; Clark 2014). This is because of the differences inherent in these groups that may impact, in a likely negative way, on the effect of MOAs. The impact may differ because of the multi‐factorial pathophysiology of constipation in people with cancer and advanced diseases (Leppert 2010). This may include structural abnormalities such as bowel obstruction; pelvic tumours; radiation fibrosis; or metabolic disturbances such as dehydration, hypercalcaemia, and hypokalaemia. It may involve neurological disorders. There may also be general issues increasing the risk and complicating the management of OIBD such as advanced age, depression, drug sedation, chemotherapy, multiple therapies, and a lack of privacy provided as an inpatient for bowel evacuation. As the person's disease progresses, they may have increasing frailty, lower activity, reduced appetite, and eventually multiple organ failure, all of which may impact on bowel function (Bader 2012). Moreover, because of these factors, people with cancer and particularly people at a palliative care stage may have a higher risk than other, less ill populations of experiencing adverse events from MOAs. This review is an update and since its most recent publication we are aware of new trials.

Objectives

To assess for opioid‐induced bowel dysfunction (OIBD) in people with cancer and people receiving palliative care the effectiveness and safety of mu‐opioid antagonists (MOAs) versus different doses of MOAs, alternative pharmacological/non‐pharmacological interventions, placebo, or no treatment.

Methods

Criteria for considering studies for this review

Types of studies

Randomised trials are the best design to minimise bias when evaluating the effectiveness of an intervention. We included double‐blind, randomised controlled trials (RCTs) evaluating the effectiveness of MOAs, compared to a different MOA or at different doses, an alternative pharmacological or non‐pharmacological intervention, a placebo, or no treatment, for OIBD. We did not include open‐label extension phases (where both the researchers and participants know whether they are in the intervention trial arm or the comparison arm) of trials or post‐hoc analyses of trials because they are at an increased risk of bias. No language restrictions were applied. If there was no full journal publication of the trial, we included a published abstract of the trial's final results if it was of sufficient detail to be able to assess risk of bias. For additional data of any included trials we also sought to identify regulatory (e.g. European Medicines Agency, and the Pharmaceuticals and Medical Devices Agency in Japan) assessments of the manufacturer's trial data from Clinical Study Reports. 

Types of participants

Eligible trials concerned participants of any age or either sex who were:

  • people with cancer or people at a palliative stage irrespective of disease, or both;

  • all or the majority (over 95%) were on a stable opioid regimen and had OIBD that had not resolved from taking laxatives.

We included trials of populations of participants where not all fitted our eligibility criteria so long as at least 50% of the sample were people with cancer or people receiving palliative care or at an advanced stage of their disease or where they provided subgroup analysis in either of these participant groups.

We did not include trials if the MOAs for bowel dysfunction were for associated postoperative ileus (arrest of intestinal peristalsis). This is because this is not caused primarily by opioids (Marderstein 2008). We excluded trials of healthy volunteers, participants with constipation because of drug misuse, and participants with constipation arising from bowel obstruction were excluded.

Types of interventions

We included trials of interventions evaluating a MOA that were either peripherally or systemically acting, and administered at any dose and by any route. These included, for example, methylnaltrexone and naloxone. We included interventions of a MOA if they were evaluated alone or in combination with another drug, for example naloxone in combination with oxycodone.

Our comparator interventions of interest were a different MOA, MOA at different doses, an alternative pharmacological or non‐pharmacological intervention, a placebo, or no treatment.

Types of outcome measures

We set four types of primary outcomes of interest and nine secondary outcomes.

Primary outcomes

Primary outcomes of interest

Laxation response:

within 24 hours (short term),  2 weeks (medium‐term) and by patient overall assessment of bowel change at the end of the trial:

  • self/clinician report of number of spontaneous rescue‐free bowel movements (within 24 hours and two weeks, by any scale or measure);

  • patient report change in bowel status measured using for instance the three‐item Bowel Function Index (BFI), where scores above 28.8 indicate constipation, or rating via the Patient Global Impression of Change using for bowel status a single rating system of better, no change or worse (within the duration of the trial).

Effect on analgesia: within 24 hours and two weeks, by any scale or measure:

  • symptoms of opioid withdrawal such as sweating, tremor, restlessness and anxiety. This could be measured using for instance the Clinical Opioid Withdrawal Scale (COWS), where a total score of greater than five is considered elevated and clinically significant;

  • change in analgesic requirements such as a 10% increase in requirements;

  • intensity of pain however measured.

Serious adverse events as defined by trial authors.

  • number and type of adverse event.

The short‐term time point of interest is the first measurement within 24 hours post intervention treatment. This will be taken as within 24 hours of first treatment unless stated otherwise. For medium term this is the first measurement taken between day one and two weeks of intervention treatment. For serious adverse events and adverse events  the time point of interest was the duration of the trial.

Secondary outcomes

Number of participants who dropped out due to adverse events.

Other measures of laxation response: by any scale or measure:

  • complete evacuation within 24 hours and 2 weeks;

  • not straining within 24 hours and 2 weeks;

  • overall symptoms of constipation in the longer term (beyond two weeks).

Relief of other constipation‐associated symptoms: by any scale or measure:

  • abdominal cramping;

  • acid reflux;

  • bloating;

  • decreased appetite;

  • difficulty breathing because of pressure in the abdomen;

  • discomfort/pain in the abdomen;

  • hard stools;

  • inability to pass stool when feeling the urge;

  • nausea and vomiting;

  • passing gas.

Use of rescue medication for laxation.

Quality of life within 24 hours and two weeks: by a validated scale such as the European Organisation for the Research and Treatment of Cancer Quality of Life Questionnaire‐C30 (EORTC QLQ‐C30).

Participant satisfaction with bowel movements.

Participant preference on bowel treatment.

Unless stated otherwise, our time points of interest were for outcomes over the duration of the trial.

For any primary or secondary outcome, if a trial used several measurements, we selected in order of priority the:

  • overall total score or global measure;

  • one deemed by the authors as the primary measure;

  • measure the sample size calculation was based on;

  • measure with the median effect. If there was an even number of outcomes, then we selected the more conservative median effect.

Search methods for identification of studies

Electronic searches

For this update, we searched five databases. 

  • CENTRAL (Cochrane Library) Issue 12 of 12 2021 (searched from August 2017 to December 2021).

  • MEDLINE and MEDLINE in process (Ovid) August 2017 to 17 December 2021.

  • Embase (Ovid) August 2017 to 17 December 2021.

  • CINAHL (EBSCO) August 2017 to December 2021.

  • Web of Science (SCI‐Expanded and CPCI‐S) August 2017 to 18 December 2021.

The search strategies are listed in Appendix 1.

Searching other resources

We searched two clinical trials registries to October 2020 that were not available via CENTRAL:

We searched Clinicaltrials.gov and ICTRP via CENTRAL. 

We searched for any included trials for drug reports from three regulatory agency websites to October 2020:

  • US Food and Drug Administration (FDA);

  • European Medicines Agency (EMA);

  • Japanese Pharmaceutical Evaluation Division, Pharmaceutical Safety and Environmental Health Bureau (JPMA).

We searched two pharmaceutical company trials registers:

We checked references lists of included trials and any identified systematic reviews. We also undertook a forward citation search of all included trials. We checked conference proceedings of the National Cancer Research Institute (NCRI) Cancer Conference and the European Association of Palliative Care (EAPC) to October 2020. We contacted authors of any identified relevant conference abstracts to ask for full details of their trials.

We wrote to pharmaceutical companies that are known manufacturers of MOAs to obtain any trial data not available in peer‐review publications; these were AstraZeneca, Mundipharma GmbH, Progenics, Shionogi, and Valeant. For this purpose, we adapted a letter developed by authors of a previous Cochrane Review; see Appendix 2 for a copy of this letter.

Data collection and analysis

Selection of studies

Two review authors (BC, LJ) independently screened the citations identified in the database searches. Where it was unclear or likely that the studies fulfilled our inclusion criteria, we retrieved the full‐text articles. If disagreements on eligibility had occurred, we would have resolved them by discussion, or if persistent, by a third review author (PS). If necessary for further clarification such as if it was unclear whether the trial identified was completed and whether their findings were available, we sought contact with the study author or sponsor.

Data extraction and management

One review author (BC) extracted data using a standard piloted form and two other review authors checked it for agreement (LJ, VV) before entry into Review Manager [RevMan Web 2020]. In the event of disagreement, it was planned a third review author (PS) would adjudicate. We collated multiple reports of the same study, so that each study rather than each report was the unit of interest in the review. We collected characteristics of the included studies in sufficient detail to populate a table of 'Characteristics of included studies' in the full review.

We extracted the following information.

  • Study design (including methods, location, funding sources, study author declarations of interest)

  • Setting

  • Participants

  • Intervention(s), Comparator(s), Outcomes (including measures and time points)

  • Numerical data for outcomes of interest

Assessment of risk of bias in included studies

Two review authors (BC, VV) independently assessed risk of bias for each trial using the criteria outlined in the Cochrane Handbook for Systematic Reviews of Interventions (Higgins 2011), resolving any disagreements by discussion. We completed a risk of bias table for each included trial. We assessed the following.

  • Random sequence generation (checking for possible selection bias). We assessed the method used to generate the allocation sequence as: low risk of bias (any truly random process: random number table; computer random number generator); and unclear risk of bias (method used to generate sequence not clearly stated). We excluded studies using a non‐random process, which were therefore at high risk of bias (odd or even date of birth; hospital or clinic record number).

  • Allocation concealment (checking for possible selection bias). The method used to conceal allocation to interventions before assignment determines whether the intervention allocation could have been foreseen in advance of, or during, recruitment, or changed after assignment. We assessed the methods as: low risk of bias (telephone or central randomisation; consecutively‐numbered, sealed, opaque envelopes); and unclear risk of bias if the method was not clearly stated. We excluded trials that did not conceal allocation, which were therefore at high risk of bias (which may be described as open list or open label).

  • Blinding of participants and personnel (checking for possible performance bias). The methods used to blind study participants and personnel from knowledge of which intervention a participant received. We assessed methods as: low risk of bias (study states that it was blinded and describes the method used to achieve blinding, such as identical tablets matched in appearance or smell, or a double‐dummy technique); unclear risk of bias (study states that it was blinded but does not provide an adequate description of how it was achieved, or it is described as open‐label, but it is not clear what is unmasked).

  • Blinding of outcome assessment (checking for possible detection bias). The methods used to blind study participants and outcome assessors from knowledge of which intervention a participant received. We assessed the methods as: low risk of bias (study has a clear statement that outcome assessors were unaware of treatment allocation, and ideally describes how this was achieved); unclear risk of bias (study states that outcome assessors were blind to treatment allocation but lacks a clear statement on how it was achieved or it is described as open‐label, but it is not clear what is unmasked).

  • Incomplete outcome data (attrition bias). We assessed whether there was attrition bias due to the amount, nature, or handling of incomplete outcome data. We judged the trial as having low risk of attrition bias if there were no missing outcome data or the reasons for missing data were unlikely to be related to true outcome, or missing data and reasons for it were similar across trial arms, or the missing data had been imputed using appropriate methods. We judged the trial as high risk if the reason for missing outcome data were likely to be related to the outcome, with either imbalance across trial arms in numbers of reasons for missing data and if an inappropriate application of simple imputation was potentially used. We judged the trial as unclear risk if there was insufficient reporting of attrition to permit judgement of low or high risk.

  • Selective outcome reporting (checking if there was a selection of a subset of the original variables recorded on the basis of the results). We assessed selective outcome reporting, if a protocol was available, by comparing outcomes in the protocol and published report. If they were the same we assessed it as low risk in this domain; if they differed, we considered it as high risk. If a protocol was not available, then we compared the outcomes listed in the methods section of an article with the outcomes for which results were reported. If they differed, we considered the trial as high risk. If a protocol was not available and even though the outcomes listed in the methods section and the results section were the same, we considered the trial as having an unclear risk of bias in this domain. Since not all trials have a protocol available, we expected to find a number of trials in this review to be at unclear risk.

Measures of treatment effect

We analysed the data using RevMan 5.4 (RevMan 2020). For dichotomous outcomes, we report risk ratios (RRs) and 95% confidence intervals (CIs). For primary outcomes, we calculated numbers needed to treat (NNT) using the 'treat‐as‐one‐trial' method. To indicate direction of effect, we present where appropriate results as either number needed to treat for an additional beneficial outcome (NNTB) or number needed to treat for an additional harmful outcome (NNTH). For continuous outcomes, we report mean differences (MDs) and 95% CIs. If authors reported both change from baseline and post treatment scores, we preferentially reported change from baseline scores. For cross‐over trials, we only generated, as appropriate, a risk ratio (RR) or mean difference (MD) for pre‐cross‐over results. We undertook a meta‐analysis if studies were sufficiently similar in design, population, interventions and outcomes. For trials that used different methods to measure the same continuous outcome, we used standardised mean differences (SMDs) and 95% CsI.

Unit of analysis issues

In our handling of each trial analytic, we considered issues that may have impacted on findings. For these we took guidance from the Cochrane Handbook for Systematic Reviews of Interventions (Higgins 2020). These were:

  • groups of participants randomised together with the same intervention (e.g. cluster‐randomised trials);

  • participants receiving more than one intervention (e.g. cross‐over trials);

  • multiple observations for the same outcomes (such as repeated measures).

Dealing with missing data

Given the nature of this field, we anticipated there would be a significant amount of missing data as a result of trial attrition due to the death of the participant.

We planned to contact trial authors if we had found data to be missing. For trials using continuous outcomes in which SDs were not reported, and no information was available from the authors, we calculated the SDs using the standard error of the mean (SEM).

Assessment of heterogeneity

We assessed statistical heterogeneity using the I² statistic. The I² statistic is a reliable and robust test to quantify heterogeneity, since it does not depend on the number of trials or on the between‐trial variance. I² measures the extent of inconsistency among trials' results, and can be interpreted as the proportion of total variation in trial estimates that is due to heterogeneity rather than sampling error. We considered an I² value of greater than 50% to indicate substantial heterogeneity and values between 75% to 100% to indicate considerable heterogeneity (Higgins 2020). Where possible, we planned to undertake sub‐analyses or sensitivity analyses in an attempt to explain heterogeneity.

Assessment of reporting biases

To reduce the risk of reporting bias, we undertook comprehensive database and registry searches, including searches of clinical trial registers and drug regulatory agency websites. We also searched websites of, and wrote to, pharmaceutical companies that are known manufacturers of MOAs to identify any further trial data.

We planned to assess reporting biases by assessing funnel plots if there were sufficient studies for such an analysis.

Data synthesis

Where trial data were sufficiently similar (in diagnostic criteria, intervention, outcome measure, length of follow‐up, and type of analysis), we combined data in a meta‐analysis to provide a pooled effect estimate. We planned to use a fixed‐effect model. For any substantial statistical heterogeneity identified we sought to investigate the extent of heterogeneity.

Subgroup analysis and investigation of heterogeneity

Where heterogeneity was identified in a meta‐analysis, we planned as appropriate subgroup and sensitivity analysis to investigate its possible sources. Subgroup analysis explores whether the overall effect varied with different trial populations, and with the nature and content of the interventions. We planned the following subgroup analysis by excluding studies where not all participants had (1) cancer and/or (2) were receiving palliative care or being at an advanced stage of their disease.

Sensitivity analysis

If sufficient trials were available, we planned to perform, in a meta‐analysis, sensitivity analyses to explore the influence of:

  • trial quality by excluding trials that had a high risk of bias in any domain;

  • outcomes measured validated tools by excluding trials that did not use validated tools.

Summary of findings and assessment of the certainty of the evidence

Two review authors (BC, VV) independently rated the certainty of the body of evidence for the primary outcomes. We used the GRADE system to rank the certainty of the evidence using the guidelines provided in Chapter 14 of the CochraneHandbook for Systematic Reviews of Interventions (Higgins 2020), GRADEpro Handbook (Schunemann 2013) and GRADE method papers (Guyatt 2011Guyatt 2013a).

The GRADE approach uses five considerations (study limitations, consistency of effect, imprecision, indirectness, and publication bias) to assess the certainty of the body of evidence for each outcome. The GRADE system uses the following criteria for assigning grade of evidence.

  • High: we are very confident that the true effect lies close to that of the estimate of the effect.

  • Moderate: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.

  • Low: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.

  • Very low: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

The GRADE system considers study design as a marker of quality. Randomised controlled trials are considered to be high quality of evidence and can be downgraded for important limitations.

Factors that may decrease the certainty level of a body of evidence are as follows.

  • Serious or very serious study limitations (risk of bias)

  • Important or serious inconsistency of results

  • Some or major indirectness of evidence

  • Serious or very serious imprecision

We included six summary of findings tables to present the main findings for mu‐opioid antagonists compared to placebo or at a different dose in a transparent and simple tabular format. In particular, we included key information concerning the certainty of evidence, the magnitude of effect of the interventions examined, and the sum of available data on the outcomes laxation response in the short and medium terms, patient assessment of bowel change and effect on pain, specifically opioid withdrawal symptoms in the medium‐term, adverse and serious adverse events.

Results

Description of studies

See Characteristics of included studies; Characteristics of excluded studies.

Results of the search

In this update, we identified 296 unique citations. See Figure 1 for the flowchart of the screening process. We identified two new trials (Katakami 2017bLee 2017), adding these to those included in the last version resulted in a total of 10 included trials with 1343 participants (Ahmedzai 2012Bull 2015Dupoiron 2017Katakami 2017aPortenoy 2008Slatkin 2009Sykes 1996Thomas 2008).


Study flow diagram.

Study flow diagram.

For five included trials we identified regulatory assessments undertaken by theEuropean Medicines Agency (EMA), and the US Food and Drug Administration (FDA) , and the Pharmaceuticals and Medical Devices Agency in Japan of the manufacturers' Clinical Study Reports (Ahmedzai 2012Katakami 2017aKatakami 2017bSlatkin 2009Thomas 2008). Only one of the regulatory assessments provided additional data, this was for use of rescue medication (Thomas 2008). We identified two regulatory reports, but they did not provide any additional data; they are referenced under Ahmedzai 2012 for oxycodone + naloxone, and Slatkin 2009 for methylnaltrexone.

Included studies

All trials were multi‐centre parallel randomised controlled trials (RCTs), except one which was a single‐centre cross‐over RCT (Sykes 1996). Eight trials had sponsorship from a pharmaceutical company (Ahmedzai 2012Bull 2015Dupoiron 2017Katakami 2017aKatakami 2017bLee 2017Slatkin 2009Thomas 2008). Two trials involved research sites in multiple countries. In one this included sites in Australia, Czech Republic, France, Germany, Hungary, Israel, the Netherlands, Poland, and the UK (Ahmedzai 2012), and in the other France, Germany, Poland, and the UK (Dupoiron 2017). In the other trials, populations were from North America (Bull 2015Portenoy 2008Slatkin 2009Thomas 2008), Japan (Katakami 2017aKatakami 2017b), South Korea (Katakami 2017aLee 2017), and the UK (Sykes 1996). Four trials had multiple community and hospital care settings including inpatients and outpatients of a hospice or hospital, and long‐term care facilities (Bull 2015Lee 2017Slatkin 2009Thomas 2008). Three were based in the community (Ahmedzai 2012Dupoiron 2017Sykes 1996). The other three did not report the setting (Katakami 2017aKatakami 2017bPortenoy 2008).

In all trials the majority of participants had a primary diagnosis of cancer. Four trials included participants with chronic cancer pain who were not described as being at an advanced disease stage (Ahmedzai 2012Dupoiron 2017Katakami 2017aKatakami 2017b). The six other trials evaluated effects in participants with an advanced disease including cancer, and other conditions such as AIDS or circulatory disease. Where reported, authors described what they meant by advanced disease by using general terms such as terminal, end‐stage, or metastatic cancer. Nine of the trials excluded patients in situations that may affect efficacy of trial by compounding constipation such as any disease processes suggestive of abnormalities of the gastrointestinal tract, or the use of chemotherapy. In the other trial this is not stated in the exclusion criteria but the investigators ‘confirmed prior to inclusion that the constipation was caused or aggravated by opioid use' (Dupoiron 2017). 

All participants were adults. At baseline all participants were on a stable opioid regimen, and had opioid‐induced bowel dysfunction (OIBD).  Eight trials specified that the indication for opioids was pain (Ahmedzai 2012Dupoiron 2017Katakami 2017aKatakami 2017bLee 2017Portenoy 2008Slatkin 2009Thomas 2008). The other two trials did not state the indication (Bull 2015Sykes 1996). Nine  trials reported that all or the majority (90% or greater) of participants were taking regular laxatives. In the 10th trial, patients were not eligible if they had been taking regular laxatives for one or more weeks before screening (Lee 2017).

Three trials had multiple trial arms (Katakami 2017aPortenoy 2008Slatkin 2009), the others were two‐armed. The mu‐opioid antagonists (MOAs) were either compared with a placebo or with the MOA administered either at different doses or in combination with other drugs. In four trials, the MOA was subcutaneous methylnaltrexone (Bull 2015Portenoy 2008Slatkin 2009Thomas 2008). Four other trials tested oral naloxone; in one naloxone only (Sykes 1996), and in three oxycodone (an opioid) in combination with naloxone (Ahmedzai 2012Dupoiron 2017Lee 2017). The other two trials evaluated oral naldemedine (Katakami 2017aKatakami 2017b). We identified no trials that evaluated naloxegol or other MOAs.

Laxation response was measured in eight trials as self, carer or clinician report (Bull 2015Katakami 2017aKatakami 2017bLee 2017Portenoy 2008Slatkin 2009Sykes 1996Thomas 2008). Two trials measured response using the Bowel Function Index (BFI) (three items, the lower the score the better bowel function) (Ahmedzai 2012Dupoiron 2017). Effect on analgesia was measured either using self‐rated pain scores or symptoms of opioid withdrawal. To measure symptoms of opioid withdrawal, three trials used the modified Himmelsbach withdrawal scale (seven items; higher scores indicating greater severity) (Portenoy 2008Slatkin 2009Thomas 2008), and two the Clinical Opioid Withdrawal Scale (COWS) (11 items, higher scores indicating more symptoms and severity. A score greater than 36 indicates severe withdrawal) (Katakami 2017aKatakami 2017b). All trials reported the incidence of serious adverse events. 

Further details of these trials including MOAs dose and schedule, and study funding source are shown in the Characteristics of included studies tables.

Ongoing studies and studies awaiting classification

We identified four trials whose results are yet to be published, of these two are evaluating methylnaltrexone (Neefjes 2014Peppin 2013), one naloxegol (NCT03067708), and one oxycodone/naloxone (Wong 2019). We identified six for which we are awaiting classification on their eligibility; this is mainly as we have insufficient details on study population. Further details of these are in the Characteristics of ongoing studies and Characteristics of studies awaiting classification, respectively.

Excluded studies

We excluded eight trials, three because they did not include participants with cancer or at the palliative stage of a disease, three as they were not RCTs, and two as the interventions were preventive. These trials are listed in the Characteristics of excluded studies.

Risk of bias in included studies

All trials were vulnerable to a number of biases, most commonly this included an unclear risk of detection bias. See Figure 2; Figure 3.


Risk of bias graph: review authors' judgements about each risk of bias item presented as percentages across all included studies.

Risk of bias graph: review authors' judgements about each risk of bias item presented as percentages across all included studies.


Risk of bias summary: review authors' judgements about each risk of bias item for each included study.

Risk of bias summary: review authors' judgements about each risk of bias item for each included study.

Allocation

Random sequence generation

The method of randomisation sequence generation was described adequately in six trials (Ahmedzai 2012; Katakami 2017a; Katakami 2017b; Lee 2017; Slatkin 2009; Thomas 2008), and we judged them to be at low risk of bias. In four trials the risk of bias was unclear as they did not provide any details.

Allocation concealment

Three trials adequately described allocation concealment (Ahmedzai 2012; Katakami 2017b; Slatkin 2009). In seven trials the risk of bias was unclear as they did not provide any details.

Blinding

Performance bias

Four trials were at a low risk of performance bias (Katakami 2017a; Katakami 2017b; Slatkin 2009; Thomas 2008). In six trials this was unclear as they did not provide any details.

Detection bias

Two trials were at a low risk of detection bias (Katakami 2017a; Katakami 2017b). In eight trials it was unclear as they did not provide any details.

Incomplete outcome data

The risk of attrition bias was low in eight trials. In one trial it was high risk as attrition was unbalanced between the trial arms with more leaving because of adverse events in the intervention arm (Katakami 2017b). In another trial risk was unclear as it was not stated how many had dropped out of the subgroup of people with cancer (Dupoiron 2017).

Selective reporting

The risk of selective reporting was unclear in five trials as there were no published protocols to check.The other five were low risk of bias as they had a protocol and whose report on outcome measurements was consistent with those in the published results paper (Ahmedzai 2012Dupoiron 2017Katakami 2017aKatakami 2017bLee 2017).

Other potential sources of bias

None of serious concern.

Effects of interventions

See: Summary of findings 1 Naldemedine compared to placebo for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care; Summary of findings 2 Low dose naldemedine compared to higher doses for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care; Summary of findings 3 Naloxone compared with placebo for opioid‐induced bowel dysfunction in people with cancer and receiving palliative care; Summary of findings 4 Naloxone + oxycodone prolonged release tablets compared with oxycodone prolonged‐released tablets for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care; Summary of findings 5 Methylnaltrexone compared to placebo for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer; Summary of findings 6 Methylnaltrexone lower dose compared to higher dose for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer

The trials varied in mu‐opioid antagonists (MOA) evaluated and comparison, and how they reported the outcomes. This limited the number of combined analyses.

Naldemedine versus placebo

Two trials (418 participants) of people with cancer irrespective of disease stage evaluated the effectiveness of two weeks of oral treatment with naldemedine compared to placebo (Katakami 2017aKatakami 2017b). In one trial the oral doses of naldemedine were per arm 0.1 mg, 0.2 mg or 0.4 mg daily for two weeks (Katakami 2017a), and in the other 0.2 mg daily for two weeks (Katakami 2017b).

Primary outcomes

See summary of findings Table 1 for this comparison.

Laxation response

Response in the short term was not reported. Two trials (418 participants) reported response in the medium term (Katakami 2017aKatakami 2017b). The risk (i.e. chance) of spontaneous laxations over two weeks in those taking naldemedine was more than three times the risk for those taking placebo (risk ratio (RR) 2.00, 95% confidence interval (CI) 1.59 to 2.52, 2 trials, 418 participants, I² = 0%; number needed to treat for an additional beneficial outcome (NNTB) 3, 95% CI 3 to 4. Analysis 1.1Katakami 2017aKatakami 2017b). We judged the certainty of evidence for laxation response within two weeks to be moderate. We downgraded evidence by one level for serious limitations to the study design as one study had a high risk of attrition bias.

Patient assessment of change in bowel status was not reported.

Effect on analgesia

Short term effect on analgesia was not reported. Only one trial (112 participants) reported on opioid withdrawal symptoms in the medium term (Katakami 2017a).

Naldemedine may have little to no effect on opioid withdrawal symptoms compared to placebo in the medium term (over two weeks since first dose) (naldemedine 0.1 mg: mean difference (MD) ‐0.10, 95% CI ‐0.56 to 0.36, 1 trial, 112 participants. Analysis 1.2; naldemedine 0.2 mg: MD 0.30, 95% CI ‐0.21 to 0.81, 1 trial, 114 participants. Analysis 1.3; naldemedine 0.4 mg: MD 0.20, 95% CI ‐0.36 to 0.76, 1 trial, 112 participants. Analysis 1.4Katakami 2017a). We judged the certainty of evidence as very low. We downgraded the certainty of evidence by two levels for very serious limitations to the study design as data derived from only one study with a high risk of attrition bias and one level because of serious imprecision as data were derived from fewer than 400 participants.

Change in analgesic requirements and pain intensity were not reported.

Serious adverse events 

Two trials (418 participants) reported serious adverse events over course of follow‐up (to two weeks in Katakami 2017a; to six weeks in Katakami 2017b).

Naldemedine may have little to no impact on the risk of non‐fatal serious adverse events compared to placebo (RR 3.34, 95% CI 0.85 to 13.15, 2 trials, 418 participants, I² = 0%. Analysis 1.5Katakami 2017bKatakami 2017a). Eleven non‐fatal serious adverse events occurred in the naldemedine arms. In one trial four of the seven non‐fatal serious adverse events in the naldemedine arm were considered to be related to the study drug, these were two cases of diarrhoea, one case of vomiting and one abnormal hepatic function test (Katakami 2017b). In the other trial there were in the naldemedine arm one case of each of gastro‐intestinal haemorrhage, pneumonia, anaemia and asthenia, the investigators do not state whether they considered these events related to the study drug (Katakami 2017a). One death occurred in one trial (Katakami 2017a), and two in the other (Katakami 2017b). All three occurred in the naldemedine trial arms, the deaths were not considered to be related to naldemedine. We judged the certainty of evidence on risk of non‐fatal serious adverse events as low. We downgraded the certainty of evidence by two levels, one for serious limitations to the study design (in one study there was a high risk of attrition bias) and one level for serious imprecision (wide confidence intervals).

Number and type of adverse events 

Two trials (418 participants) reported number and type of adverse event over course of follow‐up (to two weeks in Katakami 2017a; to six weeks in Katakami 2017b).

There was over double the risk of adverse events reported in naldemedine arms compared to placebo arms (RR 1.49, 95% CI 1.19 to 1.87, 2 trials, 418 participants, I² = 0%. Analysis 1.6Katakami 2017bKatakami 2017a). We judged the certainty of evidence as moderate. We downgraded the certainty of evidence by one level for serious limitations to the study design (in one study there was a high risk of attrition bias).

The most common adverse event in both trials was diarrhoea. There was four times the risk of diarrhoea in naldemedine arms compared to placebo arms (RR 1.85, 95% CI 1.22 to 2.82, 2 trials, 419 participants, I² = 17%. Analysis 1.7Katakami 2017bKatakami 2017a).

Secondary outcomes
Number who dropped out due to adverse events 

Outcome reported in two trials over the course of follow‐up (to two weeks in Katakami 2017a; to six weeks in Katakami 2017b).

The risk of drop out of the study due to adverse events was over eight‐times greater in the naldemedine arms compared to placebo arms (RR 5.18, 95% CI 1.28 to 20.91, 2 trials, 420 participants, I² = 0%. Analysis 1.8Katakami 2017bKatakami 2017a).

Other measures of laxation responses 

Only one trial (193 participants) reported this outcome (Katakami 2017b).

There were more spontaneous laxations that felt like a complete evacuation in the naldemedine arm compared to placebo arm (MD 2.05, 95% CI 1.29 to 2.81, 1 trial, 193 participants, full data not provided. Katakami 2017b). There were more spontaneous laxations without straining in the naldemedine arm compared to placebo arm (MD 2.67, 95% CI 1.20 to 4.15, 1 trial, 193 participants, full data not provided. Katakami 2017b).

Relief of other constipation‐associated symptoms 

Only one trial (193 participants) reported this outcome (Katakami 2017b).

There was little to no difference in overall relief of symptoms (e.g. bloating, abdomen discomfort or pain) between the naldemedine arm and placebo arm at two weeks (mean change ‐0.25 naldemedine, mean change ‐0.18 placebo, P value = not significant, 1 trial, 193 participants. Full data not provided. Katakami 2017b).

Quality of life 

Only one trial (193 participants) reported this outcome (Katakami 2017b).

There was little to no difference in quality of life between the naldemedine arm and placebo arm at two weeks (mean change ‐0.25 naldemedine, mean change‐0.15 placebo, P value = 0.08, 1 trial, 193 participants. Full data not provided. Katakami 2017b).

Satisfaction with bowel movements 

Only one trial (193 participants) reported this outcome (Katakami 2017b).

There was less dissatisfaction with bowel movements in the naldemedine arm compared with placebo arm at two weeks (mean change ‐0.50 naldemedine arm, mean change ‐0.16 placebo arm, P value = 0.015, 1 trial, 193 participants. Full data not provided. Katakami 2017b).

Use of rescue medication for laxation over course of trial, and participant preference

These outcomes were not reported.

Low dose naldemedine versus higher dose naldemedine

Only one trial (225 participants) evaluated the effectiveness of two weeks of oral treatment with naldemedine at different doses, 0.1 mg, 0.2 mg, or 0.4 mg daily, in people with cancer irrespective of disease stage (Katakami 2017a).

Primary outcomes

See summary of findings Table 2 for primary outcomes.

Laxation response

Laxation response was not reported in the short term. The trial (225 participants) reported the outcome in the medium term (Katakami 2017a).

There were fewer spontaneous laxations in the naldemedine 0.1 mg arm compared with higher dose arms of naldemedine 0.2 mg and 0.4 mg over two weeks ( 0.1 mg versus 0.4 mg: RR 0.69, 95% CI 0.53 to 0.89 1 trial, 111 participants. Analysis 2.1; 0.1 mg versus 0.2 mg: RR 0.73, 95% CI 0.55 to 0.95, 1 trial, 113 participants. Analysis 2.2). There was little to no difference in risk of spontaneous laxations between naldemedine 0.2 mg arm compared to naldemedine 0.4 mg arm (RR 0.94, 95% CI 0.79 to 1.14, 114 participants. Analysis 2.3). We judged the certainty of evidence on laxation response as low. We reduced it by one level because of serious study limitations because of unclear risk of bias (reporting bias) and one level because of serious imprecision (data derived from fewer than 400 participants).

Patient assessment of change in bowel status was not reported.

Effect on analgesia

Effect in short term was not reported. The trial (225 participants) reported opioid withdrawal symptoms in the medium term (Katakami 2017a).

There was little to no difference on opioid withdrawal symptoms between the three naldemedine dose arms (0.1 mg versus 0.2 mg. MD ‐0.40, 95% CI ‐0.90 to 0.10, 114 participants. Analysis 2.5; 0.1 mg versus 0.4 mg MD ‐0.30, 95% CI ‐0.85 to 0.25, 112 participants. Analysis 2.4;  0.2 mg versus 0.4 mg: MD 0.10, 95% CI ‐0.49 to 0.69, 114 participants.Analysis 2.6).  We judged the certainty of evidence for effect on analgesia (opioid withdrawal) to be low. We downgraded the certainty of evidence by one level for serious limitations to the study design unclear risk of bias (reporting bias) and imprecision (data derived from fewer than 400 participants). 

Change in analgesic requirements and pain intensity were not reported.

Serious adverse events 

One trial (225 participants) reported this outcome (Katakami 2017a).

There was little to no difference in occurrence of serious adverse events between the dose arms (0.1 mg versus 0.4 mg RR 0.25, 95% CI 0.03 to 2.17, 112 participants (Analysis 2.10). There were five serious adverse events. Four of the events occurred in the highest dose arm (naldemedine 0.4 mg). One participant each experienced pneumonia, anaemia, or asthenia. One participant died due to bile duct cancer. The other participant experienced a gastrointestinal bleed (taking naldemedine 0.1 mg). The investigators considered the death unrelated to the study drug. Judgements on whether the other events were related to the study drug were not reported. We judged the certainty of evidence for serious adverse events to be low. We downgraded the certainty of evidence by two levels, one for serious limitations to the study design and one for serious imprecision. This was because of unclear risk of bias (reporting bias) and a limited number of events.

Number and type of adverse events 

The trial (225 participants) reported these outcomes (Katakami 2017a).

There was little to no difference in the occurrence of an adverse event between the three naldemedine dose arms (0.1 mg versus 0.4 mg RR 0.84, 95% CI 0.67 to 1.06, 1 trial, 112 participants. Analysis 2.7; 0.1 mg versus 0.2 mg RR 0.98, 95% CI 0.76 to 1.27, 1 trial, 114 participants Analysis 2.8; 0.2 mg versus 0.4 mg RR 0.86, 95% CI 0.68 to 1.07, 1 trial, 114 participants. Analysis 2.9). We judged the certainty of evidence on risk of an adverse event to be low. We downgraded the certainty of evidence by one level for serious limitations to the study design and one level for serious imprecision. This was because of unclear risk of bias (reporting bias) and data derived from fewer than 400 participants).

The most common adverse event was diarrhoea. There were fewer events of diarrhoea in the naldemedine 0.1 mg arm compared with the naldemedine 0.4 mg arm (RR 0.61, 95% CI 0.40 to 0.95, 1 trial, 112 participants. Analysis 2.11). There was little to no difference in the proportion experiencing diarrhoea between naldemedine 0.1 mg arm and naldemedine 0.2 mg arm (RR 0.73, 95% CI 0.46 to 1.15, 1 trial, 114 participants. Analysis 2.12) and between 0.2 mg naldemedine arm and 0.4 mg naldemedine arm (RR 0.84, 95% CI 0.59 to 1.21, 1 trial, 114 participants. Analysis 2.13).

Secondary outcomes
Number who dropped out due to adverse events 

The trial (225 participants) reported this outcome (Katakami 2017a).

There was little to no difference in the proportion of participants who dropped out of the study due to adverse events between naldemedine dose arms (e.g. 0.1 mg versus 0.4 mg MD 0.75, 95% CI 0.18 to 3.20, 1 trial, 112 participants Analysis 2.14Analysis 2.15Analysis 2.16).

Other measures of laxation response 

The trial (225 participants) reported this outcome (Katakami 2017a).

There was a lower frequency of spontaneous laxations without straining in the naldemedine 0.4 mg arm compared with either of the two arms of naldemedine at lower doses (0.2 mg P value 0.04; 0.1 mg P value = < 0.001, full data not provided). There was little to no difference in the frequency without straining of spontaneous laxations between naldemedine 0.1 mg and 0.2 mg (P value = 0.16, full data not provided). There was a greater feeling of complete evacuation in naldemedine arms 0.4 mg (P value = < 0.001) and 0.2 mg (P value = 0.04) arms compared to naldemedine 0.1 mg arm (full data not provided). There was little to no difference in the feeling of complete evacuation between naldemedine arms taking either 0.4 mg or 0.2 mg (P value = 0.12, full data not provided).

Other secondary outcomes

Relief of other constipation‐associated symptoms, use of rescue medication for laxation, satisfaction with bowel movements, quality of life, and participant preference were not reported.

Naloxone versus placebo

Only one cross‐over trial (17 participants) evaluated the effectiveness of oral naloxone compared with placebo in people with advanced cancer (Sykes 1996). The participants received two days of either placebo or naloxone followed by another two days on the trial agent that was not received on day one and two. This was without washout, as in there was no treatment phase designed to reduce biased results by separating the two treatment phases of the trial to eliminate 'carry‐over' effects from the first trial drug, placebo or naloxone.  Naloxone was given four‐hourly for a total daily dose of 0.5%, 1%, 2%, 5%, 10%, or 20% of the total daily dose of morphine.

Primary outcomes

See summary of findings Table 3.

Laxation response

This outcome was not reported.

Effect on analgesia

The trial (17 participants) reported in the medium term opioid withdrawal symptoms and pain intensity (Sykes 1996). There was little to no difference in pain intensity experienced between when the participants were taking naloxone and placebo. Full data not provided, including pre‐cross‐over results provided. There was insufficient evidence provided to make a GRADE judgement on certainty of evidence. 

Change in analgesic requirements was not reported.

Serious adverse events 

The trial (17 participants) reported on this outcome (Sykes 1996). There were no serious adverse events reported. We judged the certainty of evidence on risk for a serious adverse event to be very low. We downgraded the certainty of evidence on risk by one level for serious limitations to the study design and two levels for very serious imprecision. This was because of unclear risk of bias (reporting bias) and data derived from fewer than 400 participants.

Number and type of adverse events

These outcomes were not reported.

Secondary outcomes
Number who dropped out due to adverse events 

The trial (17 participants) reported this outcome (Sykes 1996).

Four participants dropped out due to adverse events. Two participants withdrew from the study whilst taking naloxone, one because of general deterioration in health while taking naloxone (although not thought to be a causal relationship), and one participant withdrew because of nausea after two doses of naloxone at the 10% level (5 mg in this case).  One participant because of diarrhoea experienced while receiving the placebo. One participant withdrew because of severe diarrhoea caused by the lactulose taken as part of the test on bowel function.

Other outcomes

Other measures of laxation response, relief of other constipation‐associated symptoms, use of rescue medication for laxation, quality of life, patient satisfaction with bowel movements, and participant preference were not reported.

Naloxone with oxycodone versus oxycodone

Three trials (368 participants) evaluated the effectiveness of oxycodone with naloxone prolonged‐release tablets (OXN PR) compared with oxycodone prolonged‐release (OXY PR) tablets in people with cancer (Ahmedzai 2012Dupoiron 2017Lee 2017). In one trial, participants had cancer at any stage and the drug dose for OXN PR was up to 120 mg daily over four weeks of treatment (Ahmedzai 2012). In one of the other trials they evaluated five weeks of OXN PR up to 160 mg daily in people with cancer and non‐cancer pain. We included the trial's participant subset data on 46 people with cancer (Dupoiron 2017). The third trial evaluated four weeks of OXN PR up to 80 mg daily in participants with moderate to severe cancer pain (Lee 2017).

Primary outcomes

See summary of findings Table 4 for primary outcomes.

Laxation response

Risk of spontaneous rescue‐free laxations was not reported in the short or medium term.

Two trials (212 participants) reported patient assessment of change in bowel status over the course of the trial (at five weeks Ahmedzai 2012, and at four weeks since start of treatment Lee 2017). In one trial there was more improvement in bowel status in the OXN PR arm compared to OXY PR arm (mean change – 11.14, 95% CI ‐19.03 to ‐3.24, 1 trial, 133 participants, full data not provided Ahmedzai 2012). In the other there was little to no change in bowel status between trial arms (P value = 0.264, 1 trial, 79 participants, full data not provided Lee 2017). We judged the certainty of evidence on patient assessment of change in bowel status as low. We downgraded by one level because of serious limitations to the study design (unclear risk of reporting bias), and one level for serious imprecision (data derived from fewer than 400 participants). 

Effect on analgesia

Short‐term effects were not reported. Only one trial (133 participants) reported opioid withdrawal symptoms in the medium term (Ahmedzai 2012).

There was little to no difference in opioid withdrawal symptoms between OXN PR arm and OXY PR arm at one week following end of treatment (MD ‐0.63, 95% CI ‐2.44 to 1.18 , 1 trial, 133 participants. Analysis 3.1). We judged the certainty of evidence on opioid withdrawal symptoms as low.  We downgraded by one level because of serious study limitations (unclear risk of bias reporting bias) and one level for serious imprecision (data derived from fewer than 400 participants).

Medium‐term effect on change in analgesic requirements and pain intensity were not reported.

Serious adverse events 

Three trials (362 participants) reported this outcome (Ahmedzai 2012Dupoiron 2017Lee 2017).

There was little to no difference in the proportion of participants experiencing a serious adverse event (SAE) between OXN PR arms and OXY PR arms (RR 0.68, 95% CI 0.44 to 1.06) I² = 55%, 3 trials, 362 participants. Analysis 3.2). We were unable to explore the substantial statistical heterogeneity found as none of the trials fitted our criteria for either subgroup or sensitivity analyses. One trial attributed all 12 events to the study drugs; there were eight events in the OXN PR arm and four in the OXY PR arm (Ahmedzai 2012). In the other trials, one attributed none of the events to the study drug (Dupoiron 2017) and the other does not detail whether the events could be attributed to the study drug (Lee 2017). In one trial 18 participants died, nine in each trial arm (Ahmedzai 2012), in one of the other trials one participant died in the OXN PR arm and three in the OXY PR arm (Dupoiron 2017). None of the deaths were attributed to the trial drugs. The other trial did not report any deaths (Lee 2017). We judged the certainty of evidence of serious adverse events to be very low. We downgraded by one level because of serious study limitations (unclear risk of bias reporting bias), one for serious imprecision (data derived from fewer than 400 participants) and one for serious inconsistency (substantial unexplained heterogeneity).

Number and type of adverse events 

Three trials (362 participants) reported these outcomes (Ahmedzai 2012Dupoiron 2017Lee 2017).

There was little to no difference in the proportion of participants experiencing an adverse event between OXN PR arms and OXY PR arms (RR 1.01; 95% 0.87 to 1.18. I² = 0%; 3 trials, 362 participants. Analysis 3.3). We judged the certainty of evidence for number of adverse events to be low. We downgraded by one level because of serious study limitations (unclear risk of bias reporting bias) and one level for serious imprecision (data derived from fewer than 400 participants).

A common adverse event reported in all three trials was nausea. Fewer participants experienced nausea in the OXN PR arms compared with OXY PR arms (RR 0.55, 95% CI 0.33 to 0.94. I² = 0%; 3 trials, 362 participants. Analysis 3.4).

Secondary outcomes
Number who dropped out due to adverse events 

Two trials (312 participants) reported this outcome (Ahmedzai 2012Lee 2017).

There was little to no difference in the proportion of participants who dropped out of the study due to adverse events between the OXN PR arm and OXY PR arm (RR 1.25, 95% CI 0.73 to 2.15; 2 trials, 312 participants, I² = 58%, Analysis 3.5Ahmedzai 2012Lee 2017).

Use of rescue medication for laxation 

Two trials (220 participants) reported this outcome (Ahmedzai 2012Dupoiron 2017). There was little to no difference in the use of rescue medication (oral bisacodyl) between the OXN PR arms and OXY PR arms (SMD ‐0.27, 95% CI ‐0.53 to ‐0.00. 2 trials, 220 participants, I² = 0%. Analysis 3.6Ahmedzai 2012Dupoiron 2017).

Quality of life

Two trials (200 participants) reported this outcome (Ahmedzai 2012Lee 2017). There was little to no difference in quality of life at four weeks between the OXN PR arms and OXY PR arms (SMD 0.08, 95% CI ‐0.20 to 0.35, 2 trials, 200 participants, I² = 0%. Analysis 3.7Ahmedzai 2012Lee 2017).

Other outcomes

Relief of other constipation‐associated symptoms in the short to medium term, other measures of laxation response, participant satisfaction with bowel movements, and participant preference were not reported.

Methylnaltrexone versus placebo

Three trials (518 participants) evaluated the effectiveness of subcutaneous methylnaltrexone compared to placebo in people with advanced disease, of which the majority of participants had cancer (Bull 2015Slatkin 2009Thomas 2008).  One trial involved two active treatment arms; a single dose of either methylnaltrexone 0.15 mg/kg or 0.30 mg/kg (Slatkin 2009). The other two trials administered methylnaltrexone every other day for two weeks. One trial administered methylnaltrexone 0.15 mg/kg of bodyweight (Thomas 2008), and the other trial, with the aim of improving ease of administration, administered methylnaltrexone 8 mg to participants whose bodyweight was between 38 kg and 62 kg, or methylnaltrexone 12 mg if they weighed more than 62 kg (Bull 2015).

Primary outcomes

See summary of findings Table 5 .

Laxation response

Two trials (287 participants) reported short‐term outcome (Slatkin 2009Thomas 2008). The risk of spontaneous rescue‐free laxations within 24 hours of the first treatment dose was over three times greater in the methylnaltrexone arm compared to the placebo arm (RR 2.97, 95% CI 2.13 to 4.13. 2 trials, 287 participants, I² = 31%. NNTB 3, 95% CI 2 to 3. Analysis 4.1Slatkin 2009Thomas 2008). We judged the certainty of evidence for laxation within 24 hours of the first dose to be low. We downgraded by one level for serious study limitations (unclear risk of bias due to reporting bias) and one for serious imprecision (data from fewer than 400 participants).

Two trials (305 participants) reported medium‐term outcome. The risk of spontaneous rescue‐free laxations was more than seven times greater in the medium term in the methylnaltrexone arms compared to placebo arms (RR 8.15, 95% CI 4.76 to 13.95, 2 trials, 305 participants, I² = 47%. NNTB 2, 95% CI 2 to 2 Analysis 4.2Bull 2015Thomas 2008). We judged the certainty of evidence for laxation response over two weeks to be moderate. We downgraded by one level for serious study limitations (unclear risk of bias due to reporting bias). As the effect size was large, we did not downgrade for serious imprecision because data were derived from fewer than 400 participants.

Two trials report change in patient assessed bowel status over the course of the trial (287 participants) (Slatkin 2009Thomas 2008). Improvement in bowel status was three times greater in patients in the methylnaltrexone arms compared to placebo arms (RR 2.32, 95% CI 1.64 to 3.27, 2 trials, 287 participants. Analysis 4.3Slatkin 2009Thomas 2008). We judged the certainty of evidence for patient assessment of change in bowel status to be low. We downgraded by one level for serious study limitations (unclear risk of bias due to reporting bias) and one for serious imprecision (data from fewer than 400 participants).

Effect on analgesia

Two trials reported opioid withdrawal symptoms in the short term (287 participants) (Slatkin 2009Thomas 2008) and two trials (285 participants) in the medium‐term (Slatkin 2009Thomas 2008). Two trials (285 participants) reported on pain intensity in the short term (Slatkin 2009Thomas 2008).

There was little to no difference in effect on opioid withdrawal symptoms in the short term between methylnaltrexone arms at different doses and placebo arms (at four hours post treatment: methylnaltrexone 0.15 mg/kg MD ‐0.05, 95% CI ‐0.56 to 0.46, 1 trial, 99 participants. Analysis 4.5.  Slatkin 2009; methylnaltrexone 0.30 mg/kg MD ‐0.01, 95% CI ‐0.40 to 0.38, 1 trial, 107 participants. Analysis 4.6Slatkin 2009; in the other trial at 24 hours MD 0.00, 95% CI ‐0.46 to 0.46, 1 trial, 133 participants. Analysis 4.4Thomas 2008).

There was little to no difference in effect on opioid withdrawal symptoms between methylnaltrexone and placebo in the medium term (MD ‐0.20, 95% CI ‐0.80 to 0.40, 1 trial, 133 participants. Analysis 4.7.  Thomas 2008; methylnaltrexone 0.15 mg/kg MD ‐0.40, 95% CI ‐0.90 to 0.10, 1 trial, 99 participants;   Analysis 4.8Slatkin 2009;  methylnaltrexone 0.30 mg/kg  MD ‐0.15, 95% CI ‐0.57 to 0.27, 1 trial 107 participants Analysis 4.9Slatkin 2009). We judged the certainty of evidence for effect in short to medium term on opioid withdrawal symptoms to be low. We downgraded the certainty of evidence by one level for serious study limitations because of unclear risk of bias (reporting bias) and one for serious imprecision (data derived from fewer than 400 participants).

Those in the methylnaltrexone 0.15 mg/kg arm experienced reduced pain intensity compared to placebo in the short term (at four‐hours following the intervention) (MD ‐0.20, 95% CI ‐1.02 to 0.62, 1 trial. 133 participants. Analysis 4.10Thomas 2008). There was little to no difference in pain intensity in the short term in those in the methylnaltrexone 0.3 mg/kg arm compared to placebo (MD ‐0.25, 95% CI ‐0.91 to 0.41, 1 trial, 152 participants. Analysis 4.11Slatkin 2009).

We judged the certainty of evidence for effect on pain intensity to be low. We downgraded the certainty of evidence by two levels, one for serious study limitations (unclear risk of bias due to reporting bias) and one for serious imprecision (data derived from fewer than 400 participants).

Change in analgesic requirements was not reported.

Serious adverse events

Two trials reported this outcome (364 participants) (Bull 2015;  Thomas 2008).

There were fewer serious adverse events in those in the methylnaltrexone arm than for those in the placebo arm (RR 0.59, 95% CI 0.38 to 0.93; I² = 0%; 2 trials, 364 participants. Analysis 4.12Bull 2015Thomas 2008). In both trials, the investigators considered all serious adverse events as either not related or unlikely to be related to the trial drug. In Thomas 2008, the type of serious adverse events in the 11 participants who were receiving methylnaltrexone were: aneurysm ruptured, respiratory arrest, exacerbation of dyspnoea, suicidal ideation, aggression, malignant neoplasm progression, concomitant disease progression, myocardial ischaemia, aggravation of coronary artery disease, and aggravation of congestive heart failure. Bull 2015 did not describe the types of serious adverse events. 

Althouh one trial did not report serious adverse events occurring during the randomised phase (Slatkin 2009),  during its open‐label phase three participants experienced such an event. One participant had flushing, one participant had delirium possibly related to methylnaltrexone, and one participant had severe diarrhoea and subsequent dehydration and cardiovascular collapse considered to be related to methylnaltrexone. 

We judged the certainty of evidence for risk of a serious adverse event to be low. We downgraded the evidence by one level for study limitations (unclear risk of bias due to reporting bias) and one for serious imprecision (data derived from fewer than 400 participants).

Number and type of adverse events

Three trials  reported this outcome (518 participants) (Bull 2015Slatkin 2009Thomas 2008).

More participants in methylnaltrexone arms experienced adverse events than those in the placebo arms (RR 1.17, 95% CI 1.05 to 1.30; I² = 74% suggesting substantial heterogeneity between trials, 3 trials, 518 participants.  Analysis 4.13). We considered subgroup and sensitivity analyses to explore heterogeneity but none of the trials characteristics fulfilled any of our planned possible sources of heterogeneity. We judged the certainty of evidence for adverse events to be low. It was downgraded by two levels; one for study limitations (unclear risk of reporting bias) and one because of inconsistency due to substantial statistical heterogeneity between the trials.

Adverse events were reported as severe, this was based on data from two trials (Slatkin 2009Thomas 2008). One reported that during the trial and open‐label phase that 19 participants had severe events that were possibly related to methylnaltrexone (Slatkin 2009). In the other trial more participants in the placebo group experienced severe adverse events than in the intervention group (5/63 (8%) with methylnaltrexone versus 9/71 (13%) with placebo). The third trial did not report on severity (Bull 2015).

All three trials reported that participants in both methylnaltrexone and placebo arms experienced abdominal pain, flatulence, nausea, and vomiting (Bull 2015Slatkin 2009Thomas 2008). There were more reports of abdominal pain in the methylnaltrexone arm compared to placebo (RR 2.18, 95% CI 1.50 to 3.18, I² = 65% suggesting substantial heterogeneity between trials, 3 trials, 667 participants.  Analysis 4.14). We did not undertake a sensitivity analyses as none of the trials characteristics fulfilled any of our planned possible sources of heterogeneity. There was little to no difference between the methylnaltrexone and placebo arms in the proportion who experienced flatulence (RR 1.88, 95% CI 0.99 to 3.57,  I² = 0%, 3 trials, 667 participants.  Analysis 4.15) or who experienced vomiting (RR 0.95, 95% CI 0.55 to 1.65,  I² = 0%, 3 trials, 667 participants. Analysis 4.16). There were more reports of nausea in the methylnaltrexone arm compared to placebo (RR 1.89, 95% CI 1.26 to 2.85, I² = 0%, 3 trials, 667 participants. Analysis 4.17).

Secondary outcomes
Number who dropped out due to adverse events 

Two trials (364 participants) reported this outcome (Bull 2015Thomas 2008). There was little to no difference in the proportion of participants who dropped out of the study due to adverse events between the trial arms (RR 1.22, 95% CI 0.54 to 2.76, I² = 0%; 2 trials, 363 participants. Analysis 4.18). The other trial reported no dropouts occurred due to adverse events Slatkin 2009.

Use of rescue medication for laxation

Two trials (363 participants) reported this outcome (Bull 2015Thomas 2008). Fewer in the methylnaltrexone arm needed for rescue medication for laxation compared to placebo (RR 0.67, 95% CI 0.49 to 0.91, I² = 0%; 2 trials, 363 participants. Analysis 4.19).

Other secondary outcomes

Other measures of laxation responses and symptoms of constipation, satisfaction with bowel treatments, quality of life and participant preference were not reported.

Low dose methylnaltrexone versus high dose methylnaltrexone

Two trials (518 participants) evaluated different dosing regimens of methylnaltrexone in people with advanced disease (Portenoy 2008Slatkin 2009). One trial, irrespective of bodyweight, explored fixed doses of methylnaltrexone 1 mg, 5 mg, 12.5 mg, or 20 mg in 33 participants (Portenoy 2008). Because of the limited number of participants in the trials, we provide outcomes for participants taking 1 mg compared to participants taking 5 mg or greater. The drug was administered on alternate days over one week. The other trial compared one dose of different dose‐ranging schedules of 0.15 mg/kg for 47 participants with 0.3 mg/kg for 55 participants (Slatkin 2009). We did not combine the data because the dosing schedules differed.

Primary outcomes

See summary of findings Table 6 for primary outcomes for methylnaltrexone 1 mg compared to methylnaltrexone 5 mg.

Laxation response

Two trials (135 participants) reported short‐term outcome. There was little to no difference in risk of spontaneous rescue‐free bowel movements within first 24 hours (at fours hours after first dose) between participants taking a lower dose to those on a higher dose (dose 1 mg compared to 5‐20 mg, RR 0.21, 95% CI 0.03 to 1.41, 1 trial, 33 participant.Analysis 5.1.Portenoy 2008; dose 0.15 mg/kg compared to 0.3 mg/kg, RR 1.06, 95% CI 0.77 to 1.46, 1 trial, 102 participants. Analysis 5.1Slatkin 2009). We judged the certainty of evidence for laxation response within 24 hours as low. We downgraded the certainty of evidence by one level for serious study limitations and one level for serious imprecision. This was because of unclear risk of bias (reporting bias) and fewer than 400 participants. 

Only one trial (26 participants) reported outcomes in the medium term (after dosing at day three) (Portenoy 2008). There was little to no difference in risk of spontaneous rescue‐free bowel movements between participants receiving 1 mg compared to participants receiving 5 mg or greater within four hours of dose on day three (day three: RR 2.91, 95% CI 0.82, 10.39; 1 trial, 26 participants. Analysis 5.2). We judged the certainty of evidence for laxation response at day three to be very low. We downgraded the certainty of evidence by one level for serious study limitations (unclear risk of reporting bias) and two for very serious imprecision (sparse data, 26 participants). Patient‐reported overall improvement in symptoms of constipation was not reported in the medium term. 

Patient‐reported assessment of change in bowel status was reported in only one trial (Slatkin 2009). There was little to no difference in improvement between dose arms at the end of the double‐blind phase (RR 0.98, 95% CI 0.71 to 1.35, 1 trial, 102 participants. Analysis 5.3). We judged the certainty of evidence for patient‐reported assessment of change in bowel status to be low. We downgraded the certainty of evidence by one level for serious study limitations and one level for serious imprecision. This was because of unclear risk of bias (reporting bias) and fewer than 400 participants. 

Effect on analgesia

Two trials (135 participants) report on effect on analgesia in the short to medium term (Portenoy 2008Slatkin 2009). There was little to no difference between trial arms in the mean change in symptoms of opioid withdrawal from baseline to four‐hour evaluation or medium term (MD ‐0.04, 95% CI ‐0.58 to 0.50, 1 trial, 102 participants. Slatkin 2009Analysis 5.4; MD ‐0.25, 95% CI ‐0.84 to 0.34, 1 trial, 102 participants. Slatkin 2009Analysis 5.5). In the other trial there was also little to no difference in the short term and medium term between trials arms in pain levels or symptoms of opioid withdrawal (data not provided) (33 participants) (Portenoy 2008).

Change in analgesic requirements was not reported.

We judged the certainty of evidence for effect on analgesia to be low. We downgraded the certainty of evidence by one level for serious study limitations and one level for serious imprecision. This was because of unclear risk of bias (reporting bias) and fewer than 400 participants.

Serious adverse events

Two trials (135 participants) reported on serious adverse events (Portenoy 2008Slatkin 2009). In one trial, 15 participants experienced a serious adverse event (Portenoy 2008). Which trial arm they were in was not reported. The events were lymphadenectomy, febrile neutropenia, depressed level of consciousness, suicide attempt, and delirium. All were considered unrelated to study drug. In the other trial, no serious adverse events occurred during the randomised trial phase, although during the open‐label phase three participants experienced such an event of which one had severe diarrhoea and subsequent dehydration and cardiovascular collapse (Slatkin 2009). These were considered to be related to the study drug. We did not judge the certainty of evidence for serious adverse events as data were not complete.

Number and type of adverse events 

Two trials reported on adverse events (135 participants) (Portenoy 2008Slatkin 2009). There was little to no difference in the occurrence of adverse events between the different dose arms in either study. We did not combine the study data as the dosing differed substantially per study (RR 1.00, 95% CI 1.00 to 1.00, 33 participants. Portenoy 2008; RR 0.90, 95% CI 0.73 to 1.13, 102 participants. Slatkin 2009). The most common adverse event in both trials and per trial arm was abdominal pain. We judged the quality of certainty for adverse events to be low. This was because of serious study limitations due to unclear risk of bias (reporting bias) and imprecision (fewer than 400 participants).

Secondary outcomes
Number who dropped out due to adverse events 

Two trials reported on this outcome (135 participants) (Portenoy 2008Slatkin 2009). In one trial, one participant in methylnaltrexone 12.5 mg arm discontinued the trial because of an adverse event (Portenoy 2008). This was an 84‐year‐old man who withdrew due to syncope. The event was transient and resolved without sequelae; the investigators assessed that it was related to the medication. This trial also reported that in the open‐label phase, after receiving three doses, a 20‐year‐old man was withdrawn from the trial due to abdominal cramping that was considered as probably related to the trial medication. In the other trial, none of the participants discontinued because of an adverse event (Slatkin 2009).

Use of rescue medication for laxation

Only one trial (33 participants) reported this outcome (Portenoy 2008). Those in methylnaltrexone 1 mg arm required a rescue laxative approximately twice as often as those in the higher dose groups of 5 mg, 12.5 mg, and 20 mg (data were not provided).

Satisfaction with bowel movements

Only one trial (33 participants) reported this outcome (Portenoy 2008). There was little to no difference in satisfaction with bowel movements between trials arms. Data were not provided.

Other secondary outcomes 

Other measures of laxation response in short to medium term and rescue‐free laxation response in the longer term, relief of other constipation‐associated symptoms, quality of life, preference were not reported.

Discussion

Summary of main results

This is an update of the review first published in 2008, and last updated in 2018. We sought to determine the effectiveness and safety of mu‐opioid antagonists (MOAs) for opioid‐induced bowel dysfunction (OIBD) in people with cancer and people receiving palliative care. Where reported (9/10) studies excluded patients in situations that may affect efficacy by compounding constipation such as any disease processes suggestive of abnormalities of the gastrointestinal tract, and chemotherapy. Five of the 10 randomised controlled trials (RCTs) included explored outcomes in cancer populations irrespective of disease stage. Two of these studies compared oral naldemedine with placebo, one of which also compared dosing regimens, and the other three compared oral prolonged‐released oxycodone/naloxone with oxycodone alone. Oral naloxone only compared with placebo was evaluated in people with advanced cancer. The other four trials compared subcutaneous methylnaltrexone either with placebo or different regimens of methylnaltrexone in palliative care populations, in which the majority of participants had advanced cancer.

Naldemedine compared with placebo in people with cancer

We found moderate‐certainty evidence that in the medium term (over two weeks) naldemedine may increase the risk of spontaneous laxations and the risk of adverse events. There was no clear evidence that it has little to no impact on opioid withdrawal symptoms or risk of serious adverse events. We found this evidence was of very low certainty on opioid withdrawal symptoms, and low for serious adverse events. Patient assessment of bowel status was not reported.

Low‐dose naldemedine compared with higher‐dose naldemedine in people with cancer

The risk of spontaneous laxations in the medium term and risk of serious adverse events may be higher when naldemedine administered at 4 mg compared to 1 mg, but we found the evidence is of low certainty. There was little to no difference in doses in the impact on opioid withdrawal symptoms or risk of adverse events, but we found the evidence was of low certainty. Patient assessment of bowel status not reported.

Naloxone compared with placebo in people with advanced cancer

There was no reported data on laxation response, patient assessment of bowel status, effect on analgesia, serious adverse events or adverse events.

Naloxone with oxycodone versus oxycodone in people with cancer

Therewere no reported data on risk of spontaneous laxations. We found low‐certainty evidence which is inconsistent in whether naloxone with oxycodone compared to oxycodone only improves patients assessment of bowel status. There was little to no difference between naloxone with oxycodone compared to oxycodone on impact on opioid withdrawal symptoms or risk of adverse events, but we found the evidence was of low certainty. We found very low‐certainty evidence that naloxone with oxycodone has little to no impact on the risk of serious adverse events.

Methylnaltrexone compared with placebo in people receiving palliative care

We found moderate‐certainty evidence that in the medium term methylnaltrexone may increase the risk of spontaneous laxations and low‐certainty evidence that it may improve patient assessment of bowel status. There was little to no difference between methylnaltrexone compared with placebo on impact on opioid withdrawal symptoms or that it increases the risk of a serious adverse event, but we found this evidence of low certainty. We found low‐certainty evidence that methylnaltrexone increases the risk of adverse events.

Methylnaltrexone 1 mg compared with 5 mg or greater

We found low‐ to very low‐certainty evidence that there was little to no difference in impact between methylnaltrexone at 1 mg compared to 5 mg or greater on laxation response in the short and medium term. There was little to no difference on patient assessment of bowel status, opioid withdrawal symptoms, and adverse events but the evidence was of low certainty. Serious adverse events were underreported.

Overall completeness and applicability of evidence

We sought trial evidence widely beyond published papers. Where available, we obtained regulatory documents; although these provided few new data.

Our review findings were limited. The trials were few and this limited our combined analyses. In some analyses, there was statistical heterogeneity across the trials. In regards to the primary outcomes, this related to adverse effects of methylnaltrexone in comparison to placebo. We did not undertake sensitivity analyses as none of the trial characteristics fulfilled our criteria for possible sources of heterogeneity. The evidence on naldemedine was from two trials from the same research group. The trial on naloxone only measured one of our four primary outcomes of interest.

The body of evidence could be argued as stronger for methylnaltrexone, as more evidence was provided on our primary outcomes of interest. It is important to reflect that this is overall of low‐certainty evidence, and in one of the four methylnaltrexone trials the assessment of impact of the drug may have been affected as participants in the placebo arm were on higher doses of opioids than those in the methylnaltrexone arm. Our analysis was more limited on methylnaltrexone dose response as we were unable to combine the studies because of different dosing schedules.

Participant outcomes were under evaluated. Only two trials assessed quality of life (Ahmedzai 2012Katakami 2017b). Few trials reported on impact of MOAs on the intensity of pain. This may be as it is hard to assess formally as it is subjective, but it is an important to measure.  There are also other outcomes that were not measured in any of these trials that earlier research suggests need further exploration. This includes whether MOAs, in particular methylnaltrexone, increase cancer survival (Janku 2015).

We found, as we did in our previous update, no completed trials that fulfilled our inclusion criteria on naloxegol, which in 2014 was approved by the FDA for use in OIBD in people without cancer. However, there are trials of naloxegol that are registered as ongoing, the most recent is from 2017 (NCT03067708). Evaluations on the development of new MOAs for OIBD, their effectiveness, and safety is an active research field. We found 11 trials in populations of people with cancer or people receiving palliative care (or both) that were in progress, awaiting assessment or were completed, but published results were not yet available at the time of publishing this review.

Quality of the evidence

None of the evidence for the primary outcomes was judged as high certainty. The certainty was mostly low or very‐low, commonly because of study limitations (because of attrition or reporting bias) alongside serious or very serious imprecision because data involved a limited or very limited number of participants/events. Some evidence, on spontaneous rescue‐free laxations and adverse events regarding naldemedine compared with placebo, was judged as moderate. It was down‐graded once because of serious risk of attrition bias. The only other outcome whose evidence was judged as moderate was spontaneous rescue‐free laxations in the medium term regarding methylnaltrexone compared with placebo; here it was downgraded because of unclear risk of reporting bias. In two instances where we were able to combine data another quality issue occurred; this was regarding inconsistency across trials because of substantial unexplained heterogeneity. This occurred in the comparison of methylnaltrexone with placebo for adverse advents and in comparison, of naloxone + oxycodone compared with oxycodone alone for serious adverse events.

Potential biases in the review process

We sought trial evidence widely, including five citation databases. We sought unpublished trial data from pharmaceutical and regulatory agencies databases. However, there are limited guidelines in how to seek unpublished data and searching regulatory agency websites is not straightforward.

We limited inclusion to trials that specified that their participants had cancer, or were in palliative care, irrespective of disease stage. This is likely to have led to a loss of data, as trials we excluded may have included people with such characteristics, but the trial papers did not provide this level of detail.

We included trials with methodological limitations. In addition, there is a potential problem due to carry‐over effects in the cross‐over designed trial (Sykes 1996), and our combined analysis was limited by the number of trials available. As different MOA time points of greatest potential differ, in any future updates primary outcome time points may be need to be reconsidered and not standardised as in this update.

Agreements and disagreements with other studies or reviews

This is an update of a Cochrane systematic review examining the evidence for MOAs, as in its last version (Candy 2018) it is looking specifically for OIBD in cancer and palliative care populations. This update identified two new trials, whilst the certainty of the evidence for naldemedine has changed, the overall conclusions have not changed from the last published version.

There are reviews that have evaluated the effect of MOAs for OIBD across different populations, although no recent Cochrane Review. One review identified 14 trials, in addition to four of the trials included in this review, they;included trials on methadone‐induced constipation and trials involving participants receiving an opioid for chronic non‐malignant pain (Ford 2013). In their meta‐analysis of 14 trials of 4101 participants the authors found the MOAs methylnaltrexone, naloxone, and alvimopan were superior to placebo for the treatment of opioid‐induced constipation. However, the numbers of adverse events were significantly more common. In a more recent review in which the authors included trials of any treatments approved for opioid‐induced constipation; these included both MOAs and the laxatives lubiprostone and prucalopride (Nee 2018). The authors identified 26 trials and came to similar conclusions on MOAs. In recognition of the heterogeneity they observed across the trials, to identify possible moderating factors they undertook sensitivity analysis and a meta‐regression. They found that treatments were more likely to be effective in study populations taking higher doses of opioids at baseline or refractory to laxatives. In this review our data is more limited preventing a repeat of their sensitivity analysis.

Study flow diagram.

Figures and Tables -
Figure 1

Study flow diagram.

Risk of bias graph: review authors' judgements about each risk of bias item presented as percentages across all included studies.

Figures and Tables -
Figure 2

Risk of bias graph: review authors' judgements about each risk of bias item presented as percentages across all included studies.

Risk of bias summary: review authors' judgements about each risk of bias item for each included study.

Figures and Tables -
Figure 3

Risk of bias summary: review authors' judgements about each risk of bias item for each included study.

Comparison 1: Naldemedine versus placebo, Outcome 1: Sponaneous rescue‐free bowel movements: Medium term

Figures and Tables -
Analysis 1.1

Comparison 1: Naldemedine versus placebo, Outcome 1: Sponaneous rescue‐free bowel movements: Medium term

Comparison 1: Naldemedine versus placebo, Outcome 2: Symptoms of opioid withdrawal: Medium term, naldemedine 0.1 mg

Figures and Tables -
Analysis 1.2

Comparison 1: Naldemedine versus placebo, Outcome 2: Symptoms of opioid withdrawal: Medium term, naldemedine 0.1 mg

Comparison 1: Naldemedine versus placebo, Outcome 3: Symptoms of opioid withdrawal: Medium term, naldemedine 0.2 mg

Figures and Tables -
Analysis 1.3

Comparison 1: Naldemedine versus placebo, Outcome 3: Symptoms of opioid withdrawal: Medium term, naldemedine 0.2 mg

Comparison 1: Naldemedine versus placebo, Outcome 4: Symptoms of opioid withdrawal: Medium term, naldemedine 0.4 mg

Figures and Tables -
Analysis 1.4

Comparison 1: Naldemedine versus placebo, Outcome 4: Symptoms of opioid withdrawal: Medium term, naldemedine 0.4 mg

Comparison 1: Naldemedine versus placebo, Outcome 5: Serious adverse events

Figures and Tables -
Analysis 1.5

Comparison 1: Naldemedine versus placebo, Outcome 5: Serious adverse events

Comparison 1: Naldemedine versus placebo, Outcome 6: Adverse events

Figures and Tables -
Analysis 1.6

Comparison 1: Naldemedine versus placebo, Outcome 6: Adverse events

Comparison 1: Naldemedine versus placebo, Outcome 7: Proportion experiencing diarrhoea

Figures and Tables -
Analysis 1.7

Comparison 1: Naldemedine versus placebo, Outcome 7: Proportion experiencing diarrhoea

Comparison 1: Naldemedine versus placebo, Outcome 8: Proportion who dropped out due to adverse events

Figures and Tables -
Analysis 1.8

Comparison 1: Naldemedine versus placebo, Outcome 8: Proportion who dropped out due to adverse events

Comparison 2: Naldemedine dose, Outcome 1: Spontaneous rescue‐free bowel movements: Medium term, naldemedine 0.1 mg versus 0.4mg

Figures and Tables -
Analysis 2.1

Comparison 2: Naldemedine dose, Outcome 1: Spontaneous rescue‐free bowel movements: Medium term, naldemedine 0.1 mg versus 0.4mg

Comparison 2: Naldemedine dose, Outcome 2: Spontaneous rescue‐free bowel movements: Medium term, naldemedine 0.1 mg versus 0.2mg naldemedine

Figures and Tables -
Analysis 2.2

Comparison 2: Naldemedine dose, Outcome 2: Spontaneous rescue‐free bowel movements: Medium term, naldemedine 0.1 mg versus 0.2mg naldemedine

Comparison 2: Naldemedine dose, Outcome 3: Spontaneous rescue‐free bowel movements: Medium term, naldemedine 0.2 mg versus naldemedine 0.4 mg

Figures and Tables -
Analysis 2.3

Comparison 2: Naldemedine dose, Outcome 3: Spontaneous rescue‐free bowel movements: Medium term, naldemedine 0.2 mg versus naldemedine 0.4 mg

Comparison 2: Naldemedine dose, Outcome 4: Symptoms of opioid withdrawal: Medium term, naldemedine 0.1 mg versus naldemedine 0.4 mg

Figures and Tables -
Analysis 2.4

Comparison 2: Naldemedine dose, Outcome 4: Symptoms of opioid withdrawal: Medium term, naldemedine 0.1 mg versus naldemedine 0.4 mg

Comparison 2: Naldemedine dose, Outcome 5: Symptoms of opioid withdrawal: Medium term, naldemedine 0.1 mg versus naldemedine 0.2 mg

Figures and Tables -
Analysis 2.5

Comparison 2: Naldemedine dose, Outcome 5: Symptoms of opioid withdrawal: Medium term, naldemedine 0.1 mg versus naldemedine 0.2 mg

Comparison 2: Naldemedine dose, Outcome 6: Symptoms of opioid withdrawal: Medium term, naldemedine 0.2 mg versus naldemedine 0.4 mg

Figures and Tables -
Analysis 2.6

Comparison 2: Naldemedine dose, Outcome 6: Symptoms of opioid withdrawal: Medium term, naldemedine 0.2 mg versus naldemedine 0.4 mg

Comparison 2: Naldemedine dose, Outcome 7: Adverse events: naldemedine 0.1 mg versus naldemedine 0.4 mg

Figures and Tables -
Analysis 2.7

Comparison 2: Naldemedine dose, Outcome 7: Adverse events: naldemedine 0.1 mg versus naldemedine 0.4 mg

Comparison 2: Naldemedine dose, Outcome 8: Adverse events: naldemedine 0.1 mg versus naldemedine 0.2 mg

Figures and Tables -
Analysis 2.8

Comparison 2: Naldemedine dose, Outcome 8: Adverse events: naldemedine 0.1 mg versus naldemedine 0.2 mg

Comparison 2: Naldemedine dose, Outcome 9: Adverse events: naldemedine 0.2 mg versus naldemedine 0.4 mg

Figures and Tables -
Analysis 2.9

Comparison 2: Naldemedine dose, Outcome 9: Adverse events: naldemedine 0.2 mg versus naldemedine 0.4 mg

Comparison 2: Naldemedine dose, Outcome 10: Serious adverse events

Figures and Tables -
Analysis 2.10

Comparison 2: Naldemedine dose, Outcome 10: Serious adverse events

Comparison 2: Naldemedine dose, Outcome 11: Diarrhoea: naldemedine 0.1 mg versus naldemedine 0.4 mg

Figures and Tables -
Analysis 2.11

Comparison 2: Naldemedine dose, Outcome 11: Diarrhoea: naldemedine 0.1 mg versus naldemedine 0.4 mg

Comparison 2: Naldemedine dose, Outcome 12: Diarrhoea: naldemedine 0.1 mg versus naldemedine 0.2 mg

Figures and Tables -
Analysis 2.12

Comparison 2: Naldemedine dose, Outcome 12: Diarrhoea: naldemedine 0.1 mg versus naldemedine 0.2 mg

Comparison 2: Naldemedine dose, Outcome 13: Diarrhoea: naldemedine 0.2 mg versus naldemedine 0.4 mg

Figures and Tables -
Analysis 2.13

Comparison 2: Naldemedine dose, Outcome 13: Diarrhoea: naldemedine 0.2 mg versus naldemedine 0.4 mg

Comparison 2: Naldemedine dose, Outcome 14: Proportion who dropped out due to adverse events: naldemedine 0.1 mg versus naldemedine 0.4 mg

Figures and Tables -
Analysis 2.14

Comparison 2: Naldemedine dose, Outcome 14: Proportion who dropped out due to adverse events: naldemedine 0.1 mg versus naldemedine 0.4 mg

Comparison 2: Naldemedine dose, Outcome 15: Proportion who dropped out due to adverse events: naldemedine 0.1 mg versus naldemedine 0.2 mg

Figures and Tables -
Analysis 2.15

Comparison 2: Naldemedine dose, Outcome 15: Proportion who dropped out due to adverse events: naldemedine 0.1 mg versus naldemedine 0.2 mg

Comparison 2: Naldemedine dose, Outcome 16: Proportion who dropped out due to adverse events: naldemedine 0.2 mg versus naldemedine 0.4 mg

Figures and Tables -
Analysis 2.16

Comparison 2: Naldemedine dose, Outcome 16: Proportion who dropped out due to adverse events: naldemedine 0.2 mg versus naldemedine 0.4 mg

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 1: Symptoms of opioid withdrawal: medium term

Figures and Tables -
Analysis 3.1

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 1: Symptoms of opioid withdrawal: medium term

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 2: Serious adverse events

Figures and Tables -
Analysis 3.2

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 2: Serious adverse events

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 3: Adverse events

Figures and Tables -
Analysis 3.3

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 3: Adverse events

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 4: Nausea

Figures and Tables -
Analysis 3.4

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 4: Nausea

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 5: Proportion who dropped out due to adverse events

Figures and Tables -
Analysis 3.5

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 5: Proportion who dropped out due to adverse events

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 6: Use of laxative rescue medication

Figures and Tables -
Analysis 3.6

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 6: Use of laxative rescue medication

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 7: Quality of life

Figures and Tables -
Analysis 3.7

Comparison 3: Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event, Outcome 7: Quality of life

Comparison 4: Methylnaltrexone versus placebo, Outcome 1: Spontaneous rescue‐free bowel movements: short term

Figures and Tables -
Analysis 4.1

Comparison 4: Methylnaltrexone versus placebo, Outcome 1: Spontaneous rescue‐free bowel movements: short term

Comparison 4: Methylnaltrexone versus placebo, Outcome 2: Spontaneous rescue‐free bowel movements: medium term

Figures and Tables -
Analysis 4.2

Comparison 4: Methylnaltrexone versus placebo, Outcome 2: Spontaneous rescue‐free bowel movements: medium term

Comparison 4: Methylnaltrexone versus placebo, Outcome 3: Patient reported improvement in bowel status: medium term

Figures and Tables -
Analysis 4.3

Comparison 4: Methylnaltrexone versus placebo, Outcome 3: Patient reported improvement in bowel status: medium term

Comparison 4: Methylnaltrexone versus placebo, Outcome 4: Opioid withdrawal symptoms: short term

Figures and Tables -
Analysis 4.4

Comparison 4: Methylnaltrexone versus placebo, Outcome 4: Opioid withdrawal symptoms: short term

Comparison 4: Methylnaltrexone versus placebo, Outcome 5: Opioid withdrawal symptoms: mean change short term, lower dose (0.15 mg/kg) methylnaltrexone

Figures and Tables -
Analysis 4.5

Comparison 4: Methylnaltrexone versus placebo, Outcome 5: Opioid withdrawal symptoms: mean change short term, lower dose (0.15 mg/kg) methylnaltrexone

Comparison 4: Methylnaltrexone versus placebo, Outcome 6: Opioid withdrawal symptoms: mean change short term, higher dose (0.30 mg/kg) methylnaltrexone

Figures and Tables -
Analysis 4.6

Comparison 4: Methylnaltrexone versus placebo, Outcome 6: Opioid withdrawal symptoms: mean change short term, higher dose (0.30 mg/kg) methylnaltrexone

Comparison 4: Methylnaltrexone versus placebo, Outcome 7: Opioid withdrawal symptoms: medium term

Figures and Tables -
Analysis 4.7

Comparison 4: Methylnaltrexone versus placebo, Outcome 7: Opioid withdrawal symptoms: medium term

Comparison 4: Methylnaltrexone versus placebo, Outcome 8: Opioid withdrawal symptoms: mean change medium term, lower dose (0.15 mg/kg) methylnaltrexone

Figures and Tables -
Analysis 4.8

Comparison 4: Methylnaltrexone versus placebo, Outcome 8: Opioid withdrawal symptoms: mean change medium term, lower dose (0.15 mg/kg) methylnaltrexone

Comparison 4: Methylnaltrexone versus placebo, Outcome 9: Opioid withdrawal symptoms: mean change medium term, lower dose (0.3 mg/kg) methylnaltrexone

Figures and Tables -
Analysis 4.9

Comparison 4: Methylnaltrexone versus placebo, Outcome 9: Opioid withdrawal symptoms: mean change medium term, lower dose (0.3 mg/kg) methylnaltrexone

Comparison 4: Methylnaltrexone versus placebo, Outcome 10: Pain intensity: short term

Figures and Tables -
Analysis 4.10

Comparison 4: Methylnaltrexone versus placebo, Outcome 10: Pain intensity: short term

Comparison 4: Methylnaltrexone versus placebo, Outcome 11: Pain intensity: Medium term

Figures and Tables -
Analysis 4.11

Comparison 4: Methylnaltrexone versus placebo, Outcome 11: Pain intensity: Medium term

Comparison 4: Methylnaltrexone versus placebo, Outcome 12: Serious adverse event

Figures and Tables -
Analysis 4.12

Comparison 4: Methylnaltrexone versus placebo, Outcome 12: Serious adverse event

Comparison 4: Methylnaltrexone versus placebo, Outcome 13: Adverse events

Figures and Tables -
Analysis 4.13

Comparison 4: Methylnaltrexone versus placebo, Outcome 13: Adverse events

Comparison 4: Methylnaltrexone versus placebo, Outcome 14: Abdominal pain

Figures and Tables -
Analysis 4.14

Comparison 4: Methylnaltrexone versus placebo, Outcome 14: Abdominal pain

Comparison 4: Methylnaltrexone versus placebo, Outcome 15: Flatulence

Figures and Tables -
Analysis 4.15

Comparison 4: Methylnaltrexone versus placebo, Outcome 15: Flatulence

Comparison 4: Methylnaltrexone versus placebo, Outcome 16: Vomiting

Figures and Tables -
Analysis 4.16

Comparison 4: Methylnaltrexone versus placebo, Outcome 16: Vomiting

Comparison 4: Methylnaltrexone versus placebo, Outcome 17: Nausea

Figures and Tables -
Analysis 4.17

Comparison 4: Methylnaltrexone versus placebo, Outcome 17: Nausea

Comparison 4: Methylnaltrexone versus placebo, Outcome 18: Dropouts due to adverse event

Figures and Tables -
Analysis 4.18

Comparison 4: Methylnaltrexone versus placebo, Outcome 18: Dropouts due to adverse event

Comparison 4: Methylnaltrexone versus placebo, Outcome 19: Use of resuce medication

Figures and Tables -
Analysis 4.19

Comparison 4: Methylnaltrexone versus placebo, Outcome 19: Use of resuce medication

Comparison 5: Methylnaltrexone dose, Outcome 1: Spontaneous rescue‐free bowel movements: short term

Figures and Tables -
Analysis 5.1

Comparison 5: Methylnaltrexone dose, Outcome 1: Spontaneous rescue‐free bowel movements: short term

Comparison 5: Methylnaltrexone dose, Outcome 2: Spontaneous rescue‐free bowel movements: medium term

Figures and Tables -
Analysis 5.2

Comparison 5: Methylnaltrexone dose, Outcome 2: Spontaneous rescue‐free bowel movements: medium term

Comparison 5: Methylnaltrexone dose, Outcome 3: Patient reported improvement in bowel status: short term

Figures and Tables -
Analysis 5.3

Comparison 5: Methylnaltrexone dose, Outcome 3: Patient reported improvement in bowel status: short term

Comparison 5: Methylnaltrexone dose, Outcome 4: Opioid withdrawal symptoms: short term

Figures and Tables -
Analysis 5.4

Comparison 5: Methylnaltrexone dose, Outcome 4: Opioid withdrawal symptoms: short term

Comparison 5: Methylnaltrexone dose, Outcome 5: Opioid withdrawal symptoms: medium term

Figures and Tables -
Analysis 5.5

Comparison 5: Methylnaltrexone dose, Outcome 5: Opioid withdrawal symptoms: medium term

Comparison 5: Methylnaltrexone dose, Outcome 6: Adverse event

Figures and Tables -
Analysis 5.6

Comparison 5: Methylnaltrexone dose, Outcome 6: Adverse event

Summary of findings 1. Naldemedine compared to placebo for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care

Naldemedine compared to placebo for opioid‐induced bowel dysfunction for people with cancer 

Patient or population: people with cancer irrespective of whether receiving palliative care and with opioid‐induced bowel dysfunction

Settings: not stated

Intervention: naldemedine

Comparison: placebo

Outcomes

Illustrative comparative risks* (95% CI)

Relative effect
(95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Placebo

Naldemedine

Laxation response: risk of spontaneous rescue‐free bowel movementsain the short termb

Not reported

Laxation response: risk of spontaneous rescue‐free bowel movementsain the medium termc

355 per 1000 

718 per 1000

RR 2.00 (1.59 to 2.52) NNTB 3 (3 to 4)

418 (2 studies)

⊕⊕⊕⊝

Moderated

 

 

Laxation response: patient assessment of change in bowel status at the end of trial

Not reported

Symptoms of opioid withdrawalein the

medium termc

Mean change in opioid withdrawal was 0.0

Mean change in opioid withdrawal was 0.1 lower 0.1 mg; 0.3 higher 0.2 mg, 0.2 higher 0.4 mg

Naldemedine 0.1 mg: MD ‐0.10 (‐0.56 to 0.36); naldemedine  0.2 mg: MD 0.30 (‐0.21 to 0.81); naldemedine  0.4 mg: MD 0.20 (‐0.36 to 0.76)d

112 in comparison with naldemedine 0.1 mg and 0.4 mg, 114 in comparison with 0.2mg (1 study)

⊕⊝⊝⊝
Very lowf,g

 

Serious adverse eventsh

13 per 1000

41 per 1000

RR 3.34 (0.85 to 13.15)

418 (2 studies)

⊕⊕⊝⊝
Lowd,i

 

Adverse events

355 per 1000

613 per 1000

RR 1.49 (1.19 to 1.87)

418 (2 studies)

⊕⊕⊕⊝

Moderated

 

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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).

RR: risk ratio; NNTB: number needed to treat for an additional beneficial outcome; MD: mean difference

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Defined in both trials as having 3 or more laxations (not induced by rescue medication) a week/who had an increase of one of more laxations (not induced by rescue medication) a week from baseline

b Within first 24 hours

c Over two weeks

d Downgraded by one level for serious study limitations because of high risk of attrition bias in one study

e Measured by the Clinical Opioid Withdrawal Scale. Lower scores indicate symptoms of lower severity. Score of 5‐12 mild, 13‐24 moderate, 25‐36 moderately severe, more than 36 severe withdrawal. Maximum score 48.
f Downgraded by two levels for very serious study limitations because all of the data were derived from only one study with a high risk of attrition bias

g Downgraded by one level for serious imprecision as data were derived from fewer than 400 participants

h Serious non‐fatal events were reported, definition of what fits this criteria was not provided

i Downgraded by one level for serious imprecision due to wide confidence intervals

Figures and Tables -
Summary of findings 1. Naldemedine compared to placebo for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care
Summary of findings 2. Low dose naldemedine compared to higher doses for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care

Low dose naldemedine compared to higher‐dose for opioid‐induced bowel dysfunction for people with cancer 

Patient or population: people with cancer irrespective of whether they are receiving palliative care and with opioid‐induced bowel dysfunction

Setting: not stated

Intervention: Naldemedine 0.1 mg daily

Comparison: Naldemedine 0.4 mg daily

Outcomes

Illustrative comparative risks* (95% CI)

Relative effect
(95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Higher dose

0.4 mg daily

Lower dose

0.1 mg daily

Laxation response: risk of spontaneous rescue‐free bowel movements in the short terma

Not reported

Laxation response: risk of spontaneous rescue‐free bowel movements in the medium termb,c

821 per 1000

564 per 1000

RR 0.69 (0.53 to 0.89)

111 (1 study)

⊕⊕⊝⊝

Lowd,e

 

Laxation response: patient assessment of change bowel status at end of trial

Not reported

Symptoms of opioid withdrawalfin the medium termb

 

Mean change in opioid withdrawal

0.2

Mean change in opioid withdrawal ‐0.3 lower

MD 

‐0.30 [‐0.85, 0.25]

112 (1 study)

 

⊕⊕⊝⊝

Lowd,e

 

Serious adverse eventsg

0.7 per 1000

0.2 per 1000

RR 0.25 (0.03, 2.17)

112 (1 study)

⊕⊕⊝⊝

Lowd.e

 

Adverse events

786 per 1000

 

660 per 1000

RR 0.84 (0.67,1.06)

112 (1 study)

⊕⊕⊝⊝

Lowd,e

 

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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; RR: risk ratio; ; MD: mean difference

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Within first 24 hours following intervention and comparison treatment

b Defined in study as having 3 or more laxations (not induced by rescue medication) a week/who had an increase of one of more laxations (not induced by reduce medication) a week from baseline

c Measured over two weeks
d Downgraded by one level for serious study limitations due to unclear risk of bias (reporting bias)

e Downgraded by one level for serious imprecision (fewer than 400 participants for continuous data or fewer than 300 events for dichotomous data).

fMeasured by the Clinical Opioid Withdrawal Scale. Lower scores indicate symptoms of lower severity. Score of 5‐12 mild, 13‐24 moderate, 25‐36 moderately severe, more than 36 severe withdrawal. Maximum score 48.

g Serious non‐fatal events were analysed, no further definition by study authors

Figures and Tables -
Summary of findings 2. Low dose naldemedine compared to higher doses for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care
Summary of findings 3. Naloxone compared with placebo for opioid‐induced bowel dysfunction in people with cancer and receiving palliative care

Naloxone compared with placebo for people with cancer and receiving palliative care with opioid‐induced bowel dysfunction

Patient or population: people with cancer and receiving palliative care with opioid‐induced bowel dysfunction

Settings: community

Intervention: naloxone

Comparison: placebo

Outcomes

Illustrative comparative risks*

Relative effect (95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Placebo

Naloxone

Laxation response: risk of spontaneous rescue‐free bowel movements in the short terma

 

 

Not reported

Laxation response: risk of spontaneous rescue‐free bowel movements in the medium termb

 

 

Not reported

Laxation response: patient assessment of change in bowel status at the end of trial

Not reported

Symptoms of opioid withdrawal in the medium term

17 (1 study) 

Full data not provided 

Serious adverse events

17 (1 study)

⊕⊝⊝⊝

Very lowc,d

No serious adverse events were reported

Adverse events

Not reported

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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).

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Within first 24 hours

b Between 1 and 14 days

Downgraded by one level for serious study limitations: unclear risk of bias (reporting bias) 

Downgraded by two levels for very serious imprecision as sparse data (17 participants)

Figures and Tables -
Summary of findings 3. Naloxone compared with placebo for opioid‐induced bowel dysfunction in people with cancer and receiving palliative care
Summary of findings 4. Naloxone + oxycodone prolonged release tablets compared with oxycodone prolonged‐released tablets for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care

Naloxone + oxycodone prolonged release tablets compared with oxycodone prolonged‐released tablets for people with cancer and opioid‐induced bowel dysfunction

Patient or population: people with cancer irrespective of whether they were receiving palliative care opioid‐induced bowel dysfunction

Settings: community

Intervention: naloxone + oxycodone prolonged‐release tablets (OXN PR)

Comparison: oxycodone prolonged‐released tablets (OXY PR)

Outcomes

Illustrative comparative risks* (95% CI)

Relative effect (95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Oxycodone (OXY PR)

Oxycodone + naloxone (OXN PR)

Laxation response: risk of spontaneous rescue‐free bowel movements in the short terma

 

 

 

Not reported

Laxation response: risk of spontaneous rescue‐free bowel movements in the medium termb

Not reported

Laxation response: Patient assessment of change in bowel statuscat the end of trial

data not provided

data not provided

Study 1: Mean change ‐ 11.14 (‐19.03, ‐3.24)

Study 2: Little to no change p value = 0.264

212 (2 studies)

⊕⊕⊝⊝

Lowd,e 

Full data not provided in either study

Symptoms of opioid withdrawalfin the medium termb

Mean 7.27

Mean 0.63 lower

MD ‐0.63 (‐2.44, 1.18)

133 (1 study)

⊕⊕⊝⊝

Lowd,e

Serious adverse eventsg

208 per 1000

141 per 1000

RR 0.68 (0.44 to 1.06)

362 (3 studies)

⊕⊝⊝⊝

Very lowd,e,h

Adverse events

584 per 1000

592 per 1000

RR 1.01 (0.87 to 1.18)

362 (3 studies)

⊕⊕⊝⊝

Lowd,e

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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; RR: risk ratio; ; MD: mean difference

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Within first 24 hours

b Between 1 and 14 days

c Measured in one study using 3‐item Bowel Function Index, where lower scores indicate better bowel function, and scores above 28.8 indicate constipation. Scores range from 0 to 100. In the other study change in bowel habits was measured using a 3‐point Likert Scale (worsened, no change, improved)

d Downgraded by one level because of serious study limitations (unclear risk of reporting bias)
e Downgraded by one level because of serious imprecision (data from fewer than 400 participants)

f Measured using the 16‐item Modified Subjective Opiate Withdrawal Scale. Lower scores indicate symptoms of lower severity. Range 0 to 64. Further scoring details not reported

g Not defined by trial authors

Downgraded by one level because of serious unexplained inconsistency (substantial heterogeneity I2 = 55%)

Figures and Tables -
Summary of findings 4. Naloxone + oxycodone prolonged release tablets compared with oxycodone prolonged‐released tablets for opioid‐induced bowel dysfunction in people with cancer irrespective of whether they were receiving palliative care
Summary of findings 5. Methylnaltrexone compared to placebo for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer

Methylnaltrexone compared to placebo for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer

Patient or population: people receiving palliative care irrespective of whether they had cancer with opioid‐induced bowel dysfunction

Setting: hospital and community

Intervention: methylnaltrexone

Comparison: placebo

Outcomes

Anticipated absolute effects* (95% CI)

Relative effect
(95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Risk with placebo

Risk with

methylnaltrexone

Laxation response: risk of spontaneous rescue‐free bowel movementsain the short termb

236 per 1000

701 per 1000 (625 to 770)

RR 2.97 (2.13 to 4.13) NNTB 3 (2 to 3)

287 (2 studies)

⊕⊕⊝⊝

Lowc,d

 

Laxation response: risk of spontaneous rescue‐free bowel movementsain the medium terme

85 per 1000

671 per 1000
(590 to 745)

RR 8.15 (4.76 to 13.95) NNTB 2 (2 to 2)

305
(2 studies)

⊕⊕⊕⊝

Moderatec,f

 

Laxation response: patient assessment of change in bowel statusgat the end of trial

252 per 1000

567 per 1000

(488 to 644)

RR 2.32 (1.64 to 3.27)*

287 (2 studies)

⊕⊕⊝⊝

Lowc,d

Proportion reporting improvement

Symptoms of opioid withdrawalhin the medium term

Mean 8.1

Mean 0.2lower

MD ‐0.20 (‐0.80 to 0.40)

133 (1 study)

⊕⊕⊝⊝

Lowc,d

 

 

Serious adverse eventsi

238 per 1000

142 per 1000
(88 to 219)

RR 0.59 (0.38 to 0.93)

364
(2 studies)

⊕⊕⊝⊝

Lowc,d

 

Adverse events

700 per 1000

797 per 1000
(745 to 869)

RR 1.17

(CI 1.05 to 1.30)

518
(3 studies)

⊕⊕⊝⊝

Lowc,j

Heterogeneity was substantial (74%). We did not undertake a sensitivity analyses as none of our predefined criteria for undertaking one were matched.

*The risk in the intervention group (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; MD: mean difference; RR: risk ratio; NNTB: number needed to treat for an additional beneficial outcome

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate: the true effect is likely to be close to the estimate of the effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited: the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate: the true effect is likely to be substantially different from the estimate of effect.

a Measured by self‐report or clinician report

b Within first 24 hours following intervention and comparison treatment

cDowngraded once for serious study limitations because of unclear risk of reporting bias

dDowngraded once for serious imprecision (data fewer than 400 participants)

eBetween 1 and 14 days

fAs the effect size was large we did not downgrade for imprecision

gMeasured in both studies using the Global Clinical Impression of Change, a scale ranging from 1 to 7, with higher scores indicating better bowel function

hMeasured using the modified Himmelsbach Opioid Withdrawal Scale. Lower scores indicate symptoms of lower severity. Total scores range from 7 to 28.
Not defined by trial authors

jDowngraded once for serious inconsistency because of substantial heterogeneity across trials

*In one trial with 2 comparisons with the same control arm, we combined the intervention groups to form a single pairwise comparison

Figures and Tables -
Summary of findings 5. Methylnaltrexone compared to placebo for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer
Summary of findings 6. Methylnaltrexone lower dose compared to higher dose for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer

Methylnaltrexone 1 mg compared to methylnaltrexone 5 mg or greater for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer

Patient or population: people receiving palliative care irrespective of whether they had cancer with opioid‐induced bowel dysfunction

Setting: hospital and community

Intervention 1: lower‐dose methylnaltrexone (study 1: 3 doses, 1 week, 1 mg; study 2: 1 dose, 0.15 mg/kg)

Intervention 2: higher‐dose methylnaltrexone (study 1: 3 doses, 1 week, 5‐20 mg; study 2: 1 dose, 0.30 mg/kg)

Outcomes

Illustrative comparative risks* (95% CI)

Relative effect
(95% CI)

No of participants
(studies)

Certainty of the evidence
(GRADE)

Comments

Assumed risk

Corresponding risk

Higher dose (5 mg)?

Lower dose (1 mg)?

Laxation response: risk of spontaneous rescue‐free bowel movementsain the short termb

Study 1: 609 per 1000

Study 2: 639 per 1000

Study 1: 499 per 1000 (250 to 100)

Study 2: 681 per 1000 (515 to 904)

Study 1: RR 0.21 (0.03 to 1.41)

Study 2: 

RR 1.06 (0.77 to 1.46)

135 (2 studies) Study 1: n = 33

Study 2: n = 102

⊕⊕⊝⊝

Lowc,d

Study data not combined as methylnaltrexone dosing differed substantially per study.

Laxation response: risk of spontaneous rescue‐free bowel movementsa,in the medium terme

647 per 1000

222per 1000 

 RR 2.91 (0.82 to 10.39)

 

26 (1 study)

⊕⊝⊝⊝

Very lowc,f

 

Laxation response: patient assessment of change in bowel statusgat the end of trial

58 per 100

60 per 1000

RR 0.98 (0.71 to 1.35)

102 (1 study)

⊕⊕⊝⊝

Lowc,d

 

Symptoms of opioid withdrawal in the medium term

0.25

mean 0.25 lower 

MD ‐0.25 (‐0.84 to 0.34)

102 (1 study)

⊕⊕⊝⊝

Lowc,d

Data not combined as methylnaltrexone dosing differed.

Serious adverse events

In one trial, 15 serious adverse events occurred during the randomised trial phase but it does not report what arm the events occurred in. 

Adverse events

Study 1: 1000 per 1000

Study 2: 800 per 1000

Study 1: 1000 per 1000 (1000 to 1000)

Study 2: 723 per 1000

(580 to 902)

Study 1: RR 1.00 (1.00 to 1.00)

Study 2: RR 0.90 (0.73 to 1.13)

135 (2 studies)

Study 1: n = 33

Study 2: n = 102

⊕⊕⊝⊝

Lowc,d

 

 

Study data not combined as methylnaltrexone dosing differed substantially per study

*The basis for the assumed risk (e.g. the median control group risk across studies) is provided in footnotes. 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; MD: mean difference; RR: risk ratio.

GRADE Working Group grades of evidence
High certainty: we are very confident that the true effect lies close to that of the estimate of the effect.
Moderate certainty: we are moderately confident in the effect estimate; the true effect is likely to be close to the estimate of effect, but there is a possibility that it is substantially different.
Low certainty: our confidence in the effect estimate is limited; the true effect may be substantially different from the estimate of the effect.
Very low certainty: we have very little confidence in the effect estimate; the true effect is likely to be substantially different from the estimate of effect.

a Measured by clinician or self‐report

b Within first 24 hours following intervention and comparison treatment

c Downgraded by one level for serious study limitations: unclear risk of bias (reporting bias)

d Downgraded by one level for serious imprecision as fewer than 400 participants.

eBetween 1 and 14 days

f Downgraded by two levels for very serious imprecision as sparse data 26 participants and wide confidence intervals

Figures and Tables -
Summary of findings 6. Methylnaltrexone lower dose compared to higher dose for opioid‐induced bowel dysfunction in people receiving palliative care irrespective of whether they had cancer
Comparison 1. Naldemedine versus placebo

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

1.1 Sponaneous rescue‐free bowel movements: Medium term Show forest plot

2

418

Risk Ratio (M‐H, Fixed, 95% CI)

2.00 [1.59, 2.52]

1.2 Symptoms of opioid withdrawal: Medium term, naldemedine 0.1 mg Show forest plot

1

112

Mean Difference (IV, Fixed, 95% CI)

‐0.10 [‐0.56, 0.36]

1.3 Symptoms of opioid withdrawal: Medium term, naldemedine 0.2 mg Show forest plot

1

114

Mean Difference (IV, Fixed, 95% CI)

0.30 [‐0.21, 0.81]

1.4 Symptoms of opioid withdrawal: Medium term, naldemedine 0.4 mg Show forest plot

1

112

Mean Difference (IV, Fixed, 95% CI)

0.20 [‐0.36, 0.76]

1.5 Serious adverse events Show forest plot

2

418

Risk Ratio (M‐H, Fixed, 95% CI)

3.34 [0.85, 13.15]

1.6 Adverse events Show forest plot

2

418

Risk Ratio (M‐H, Fixed, 95% CI)

1.49 [1.19, 1.87]

1.7 Proportion experiencing diarrhoea Show forest plot

2

419

Risk Ratio (M‐H, Fixed, 95% CI)

1.85 [1.22, 2.82]

1.8 Proportion who dropped out due to adverse events Show forest plot

2

420

Risk Ratio (M‐H, Fixed, 95% CI)

5.18 [1.28, 20.91]

Figures and Tables -
Comparison 1. Naldemedine versus placebo
Comparison 2. Naldemedine dose

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

2.1 Spontaneous rescue‐free bowel movements: Medium term, naldemedine 0.1 mg versus 0.4mg Show forest plot

1

111

Risk Ratio (M‐H, Fixed, 95% CI)

0.69 [0.53, 0.89]

2.2 Spontaneous rescue‐free bowel movements: Medium term, naldemedine 0.1 mg versus 0.2mg naldemedine Show forest plot

1

113

Risk Ratio (M‐H, Fixed, 95% CI)

0.73 [0.55, 0.95]

2.3 Spontaneous rescue‐free bowel movements: Medium term, naldemedine 0.2 mg versus naldemedine 0.4 mg Show forest plot

1

114

Risk Ratio (M‐H, Fixed, 95% CI)

0.94 [0.79, 1.14]

2.4 Symptoms of opioid withdrawal: Medium term, naldemedine 0.1 mg versus naldemedine 0.4 mg Show forest plot

1

112

Mean Difference (IV, Fixed, 95% CI)

‐0.30 [‐0.85, 0.25]

2.5 Symptoms of opioid withdrawal: Medium term, naldemedine 0.1 mg versus naldemedine 0.2 mg Show forest plot

1

114

Mean Difference (IV, Fixed, 95% CI)

‐0.40 [‐0.90, 0.10]

2.6 Symptoms of opioid withdrawal: Medium term, naldemedine 0.2 mg versus naldemedine 0.4 mg Show forest plot

1

114

Mean Difference (IV, Fixed, 95% CI)

0.10 [‐0.49, 0.69]

2.7 Adverse events: naldemedine 0.1 mg versus naldemedine 0.4 mg Show forest plot

1

112

Risk Ratio (M‐H, Fixed, 95% CI)

0.84 [0.67, 1.06]

2.8 Adverse events: naldemedine 0.1 mg versus naldemedine 0.2 mg Show forest plot

1

114

Risk Ratio (M‐H, Fixed, 95% CI)

0.98 [0.76, 1.27]

2.9 Adverse events: naldemedine 0.2 mg versus naldemedine 0.4 mg Show forest plot

1

114

Risk Ratio (M‐H, Fixed, 95% CI)

0.86 [0.68, 1.07]

2.10 Serious adverse events Show forest plot

1

112

Risk Ratio (M‐H, Fixed, 95% CI)

0.25 [0.03, 2.17]

2.11 Diarrhoea: naldemedine 0.1 mg versus naldemedine 0.4 mg Show forest plot

1

112

Risk Ratio (M‐H, Fixed, 95% CI)

0.61 [0.40, 0.95]

2.12 Diarrhoea: naldemedine 0.1 mg versus naldemedine 0.2 mg Show forest plot

1

114

Risk Ratio (M‐H, Fixed, 95% CI)

0.73 [0.46, 1.15]

2.13 Diarrhoea: naldemedine 0.2 mg versus naldemedine 0.4 mg Show forest plot

1

114

Risk Ratio (M‐H, Fixed, 95% CI)

0.84 [0.59, 1.21]

2.14 Proportion who dropped out due to adverse events: naldemedine 0.1 mg versus naldemedine 0.4 mg Show forest plot

1

112

Risk Ratio (M‐H, Fixed, 95% CI)

0.75 [0.18, 3.20]

2.15 Proportion who dropped out due to adverse events: naldemedine 0.1 mg versus naldemedine 0.2 mg Show forest plot

1

114

Risk Ratio (M‐H, Fixed, 95% CI)

3.11 [0.33, 28.99]

2.16 Proportion who dropped out due to adverse events: naldemedine 0.2 mg versus naldemedine 0.4 mg Show forest plot

1

114

Risk Ratio (M‐H, Fixed, 95% CI)

0.24 [0.03, 2.09]

Figures and Tables -
Comparison 2. Naldemedine dose
Comparison 3. Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

3.1 Symptoms of opioid withdrawal: medium term Show forest plot

1

133

Mean Difference (IV, Fixed, 95% CI)

‐0.63 [‐2.44, 1.18]

3.2 Serious adverse events Show forest plot

3

362

Risk Ratio (M‐H, Fixed, 95% CI)

0.68 [0.44, 1.06]

3.3 Adverse events Show forest plot

3

362

Risk Ratio (M‐H, Fixed, 95% CI)

1.01 [0.87, 1.18]

3.4 Nausea Show forest plot

3

362

Risk Ratio (M‐H, Fixed, 95% CI)

0.55 [0.33, 0.94]

3.5 Proportion who dropped out due to adverse events Show forest plot

2

312

Risk Ratio (M‐H, Fixed, 95% CI)

1.25 [0.73, 2.15]

3.6 Use of laxative rescue medication Show forest plot

2

220

Std. Mean Difference (IV, Fixed, 95% CI)

‐0.27 [‐0.53, ‐0.00]

3.7 Quality of life Show forest plot

2

200

Std. Mean Difference (IV, Fixed, 95% CI)

0.08 [‐0.20, 0.35]

Figures and Tables -
Comparison 3. Naloxone/oxycodone prolonged‐release tablets versus oxycodone prolonged‐release: adverse event
Comparison 4. Methylnaltrexone versus placebo

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

4.1 Spontaneous rescue‐free bowel movements: short term Show forest plot

2

287

Risk Ratio (M‐H, Fixed, 95% CI)

2.97 [2.13, 4.13]

4.2 Spontaneous rescue‐free bowel movements: medium term Show forest plot

2

305

Risk Ratio (M‐H, Fixed, 95% CI)

8.15 [4.76, 13.95]

4.3 Patient reported improvement in bowel status: medium term Show forest plot

2

287

Risk Ratio (M‐H, Fixed, 95% CI)

2.32 [1.64, 3.27]

4.4 Opioid withdrawal symptoms: short term Show forest plot

1

133

Mean Difference (IV, Fixed, 95% CI)

0.00 [‐0.46, 0.46]

4.5 Opioid withdrawal symptoms: mean change short term, lower dose (0.15 mg/kg) methylnaltrexone Show forest plot

1

99

Mean Difference (IV, Fixed, 95% CI)

‐0.05 [‐0.56, 0.46]

4.6 Opioid withdrawal symptoms: mean change short term, higher dose (0.30 mg/kg) methylnaltrexone Show forest plot

1

107

Mean Difference (IV, Fixed, 95% CI)

‐0.01 [‐0.40, 0.38]

4.7 Opioid withdrawal symptoms: medium term Show forest plot

1

133

Mean Difference (IV, Fixed, 95% CI)

‐0.20 [‐0.80, 0.40]

4.8 Opioid withdrawal symptoms: mean change medium term, lower dose (0.15 mg/kg) methylnaltrexone Show forest plot

1

99

Mean Difference (IV, Fixed, 95% CI)

‐0.40 [‐0.90, 0.10]

4.9 Opioid withdrawal symptoms: mean change medium term, lower dose (0.3 mg/kg) methylnaltrexone Show forest plot

1

107

Mean Difference (IV, Fixed, 95% CI)

‐0.15 [‐0.57, 0.27]

4.10 Pain intensity: short term Show forest plot

1

133

Mean Difference (IV, Fixed, 95% CI)

‐0.20 [‐1.02, 0.62]

4.11 Pain intensity: Medium term Show forest plot

2

Mean Difference (IV, Fixed, 95% CI)

Subtotals only

4.12 Serious adverse event Show forest plot

2

364

Risk Ratio (M‐H, Fixed, 95% CI)

0.59 [0.38, 0.93]

4.13 Adverse events Show forest plot

3

518

Risk Ratio (M‐H, Fixed, 95% CI)

1.17 [1.05, 1.30]

4.14 Abdominal pain Show forest plot

3

667

Risk Ratio (M‐H, Fixed, 95% CI)

2.18 [1.50, 3.18]

4.15 Flatulence Show forest plot

3

667

Risk Ratio (M‐H, Fixed, 95% CI)

1.88 [0.99, 3.57]

4.16 Vomiting Show forest plot

3

667

Risk Ratio (M‐H, Fixed, 95% CI)

0.95 [0.55, 1.65]

4.17 Nausea Show forest plot

3

667

Risk Ratio (M‐H, Fixed, 95% CI)

1.89 [1.26, 2.85]

4.18 Dropouts due to adverse event Show forest plot

2

363

Risk Ratio (M‐H, Fixed, 95% CI)

1.22 [0.54, 2.76]

4.19 Use of resuce medication Show forest plot

2

363

Risk Ratio (M‐H, Fixed, 95% CI)

0.67 [0.49, 0.91]

Figures and Tables -
Comparison 4. Methylnaltrexone versus placebo
Comparison 5. Methylnaltrexone dose

Outcome or subgroup title

No. of studies

No. of participants

Statistical method

Effect size

5.1 Spontaneous rescue‐free bowel movements: short term Show forest plot

2

Risk Ratio (M‐H, Fixed, 95% CI)

Subtotals only

5.2 Spontaneous rescue‐free bowel movements: medium term Show forest plot

1

26

Risk Ratio (M‐H, Fixed, 95% CI)

2.91 [0.82, 10.39]

5.3 Patient reported improvement in bowel status: short term Show forest plot

1

102

Risk Ratio (M‐H, Fixed, 95% CI)

0.98 [0.71, 1.35]

5.4 Opioid withdrawal symptoms: short term Show forest plot

1

102

Mean Difference (IV, Fixed, 95% CI)

‐0.04 [‐0.58, 0.50]

5.5 Opioid withdrawal symptoms: medium term Show forest plot

1

102

Mean Difference (IV, Fixed, 95% CI)

‐0.25 [‐0.84, 0.34]

5.6 Adverse event Show forest plot

2

Risk Ratio (M‐H, Fixed, 95% CI)

Subtotals only

Figures and Tables -
Comparison 5. Methylnaltrexone dose