作为炎症性肠病诱导疗法的生物疗法和小分子疗法试验中安慰剂的危害:系统回顾和荟萃分析。

IF 30.9 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Lancet Gastroenterology & Hepatology Pub Date : 2024-11-01 Epub Date: 2024-09-20 DOI:10.1016/S2468-1253(24)00264-4
Shahida Din, Jonathan Segal, Jonathan Blackwell, Beatriz Gros, Christopher J Black, Alexander C Ford
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引用次数: 0

摘要

背景:随机安慰剂对照试验是评估溃疡性结肠炎和克罗恩病新型药物的黄金标准。然而,接受安慰剂可能会带来风险。我们的目的是通过一项荟萃分析,研究在用于诱导溃疡性结肠炎和腔道克罗恩病缓解的许可生物制剂和小分子药物试验中接受安慰剂的相关危害:我们进行了系统回顾和荟萃分析。我们检索了MEDLINE、Embase、Embase Classic和Cochrane对照试验中央注册库中从数据库开始到2024年5月30日的所有研究,以寻找针对中度至重度活动性溃疡性结肠炎或腔隙性克罗恩病成人(≥18岁)的许可生物制剂和小分子药物诱导缓解的随机安慰剂对照试验,这些试验报告了至少4周治疗期间的不良事件数据。没有预先规定研究排除标准。我们提取了汇总数据,并采用随机效应模型对任何治疗引发的不良事件、任何药物相关不良事件、感染、炎症性肠病 (IBD) 活动恶化、因不良事件而停药、严重不良事件、严重感染、IBD 活动严重恶化或静脉血栓栓塞事件 (VTE) 进行了汇总,报告了相对风险系数 (RR) 及 95% CI。该荟萃分析方案已在 PROSPERO(CRD42024527341)注册:搜索结果发现了 10 826 篇引文,其中 47 项试验包括 20 987 名患者(14 267 名患者[68-0%]接受活性药物治疗,6720 名患者[32-0%]接受安慰剂治疗)符合条件。使用活性药物与使用安慰剂相比,发生任何治疗突发不良事件的风险均无差别(使用活性药物的患者为 7660/14 267 [53-7%] vs 使用安慰剂的患者为 3758/6720 [55-9%];RR 0-97,95% CI 0-94-1-00;I2 =36%)。然而,IBD 活动性恶化(563/13 473 [4-2%] vs 530/6252 [8-5%];0-48,0-40-0-59;I2 =54%)、因不良事件而停药(401/13 363 [3-0%] vs 299/6267 [4-8%],0-62,0-48-0-59;I2 =54%)的风险较低;0-62,0-48-0-79;I2 =46%)、严重不良事件(682/14 267 [4-8%] vs 483/6720 [7-2%];0-69,0-59-0-80;I2 =30%)、严重感染(140/14 194 [1-0%] vs 91/6647 [1-4%];0-67,0-50-0-89;I2 =0%)、IBD 活动严重恶化(187/11 271 [1-7%] vs 189/5056 [3-7%];0-45, 0-34-0-60; I2 =27%)或 VTEs(13/7542 [0-2%] vs 12/2981 [0-4%]; 0-45, 0-21-0-94; I2 =0%)均显著低于安慰剂。为避免这些潜在的严重不良事件,使用活性药物所需的治疗人数从 23 人(IBD 活动恶化)到 452 人(VTEs)不等。27项随机对照试验在所有领域均被判定为低偏倚风险:解释:接受安慰剂治疗的中度至重度活动性 IBD 患者更有可能出现 IBD 活动明显恶化和一些严重不良事件,这可能与使用活性药物降低了这些事件的风险有关。应就这些潜在危害向患者提供咨询,并考虑采用其他试验设计来减轻这些危害:无。
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Harms with placebo in trials of biological therapies and small molecules as induction therapy in inflammatory bowel disease: a systematic review and meta-analysis.

Background: Randomised placebo-controlled trials are the gold standard to assess novel drugs in ulcerative colitis and Crohn's disease. However, there might be risks associated with receiving placebo. We aimed to examine the harms associated with receiving placebo in trials of licensed biologics and small molecules for the induction of remission in ulcerative colitis and luminal Crohn's disease in a meta-analysis.

Methods: We performed a systematic review and meta-analysis. We searched MEDLINE, Embase, Embase Classic, and the Cochrane Central Register of Controlled Trials from database inception to May 30, 2024, for randomised placebo-controlled trials of licensed biologics and small molecules for induction of remission in adults (≥18 years) with moderately to severely active ulcerative colitis or luminal Crohn's disease reporting data on adverse events over a minimum treatment period of 4 weeks. There were no prespecified study exclusion criteria. We extracted summary data and pooled data using a random-effects model for any treatment-emergent adverse event, any drug-related adverse event, infection, worsening of inflammatory bowel disease (IBD) activity, withdrawal due to adverse events, serious adverse events, serious infection, serious worsening of IBD activity, or venous thromboembolic events (VTEs), reporting relative risks (RRs) with 95% CIs. The protocol for this meta-analysis was registered with PROSPERO (CRD42024527341).

Findings: The search identified 10 826 citations, of which 47 trials including 20 987 patients (14 267 [68·0%] receiving active drug and 6720 [32·0%] receiving placebo) were eligible. The risk of any treatment-emergent adverse event was no different with active drug than with placebo (7660/14 267 [53·7%] patients on active drug vs 3758/6720 [55·9%] on placebo; RR 0·97, 95% CI 0·94-1·00; I2 =36%). However, the risks of worsening of IBD activity (563/13 473 [4·2%] vs 530/6252 [8·5%]; 0·48, 0·40-0·59; I2 =54%), withdrawal due to adverse event (401/13 363 [3·0%] vs 299/6267 [4·8%]; 0·62, 0·48-0·79; I2 =46%), serious adverse event (682/14 267 [4·8%] vs 483/6720 [7·2%]; 0·69, 0·59-0·80; I2 =30%), serious infection (140/14 194 [1·0%] vs 91/6647 [1·4%]; 0·67, 0·50-0·89; I2 =0%), serious worsening of IBD activity (187/11 271 [1·7%] vs 189/5056 [3·7%]; 0·45, 0·34-0·60; I2 =27%), or VTEs (13/7542 [0·2%] vs 12/2981 [0·4%]; 0·45, 0·21-0·94; I2 =0%) were all significantly lower with active drug than placebo. Numbers needed to treat with active drug to avoid these potentially serious adverse events ranged from 23 for worsening of IBD activity to 452 for VTEs. 27 randomised controlled trials were judged as low risk of bias across all domains.

Interpretation: Patients with moderately to severely active IBD receiving placebo are more likely to experience significant worsening of IBD activity and some serious adverse events, which might relate to a reduction in risk of these events with active drug. Patients should be counselled about these potential harms, and alternative trial designs to mitigate these harms should be considered.

Funding: None.

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来源期刊
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期刊介绍: The Lancet Gastroenterology & Hepatology is an authoritative forum for key opinion leaders across medicine, government, and health systems to influence clinical practice, explore global policy, and inform constructive, positive change worldwide. The Lancet Gastroenterology & Hepatology publishes papers that reflect the rich variety of ongoing clinical research in these fields, especially in the areas of inflammatory bowel diseases, NAFLD and NASH, functional gastrointestinal disorders, digestive cancers, and viral hepatitis.
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