Sepúlveda Andrea, de la Piedra Bustamante Maria Jose, Orlanski-Meyer Esther, Villarroel Del Pino Luis A, Olivares Labbe Maria Teresa, Gana Juan Cristóbal
Department of Gastroenterology and Nutrition, Division of Pediatrics, School of Medicine, Pontificia Universidad Católica de Chile, Santiago, Chile.
The Juliet Keidan Institute of Pediatric Gastroenterology and Nutrition, Shaare Zedek Medical Center, Jerusalem, Israel.
Cochrane Database Syst Rev. 2025 Aug 1;8(8):CD014497. doi: 10.1002/14651858.CD014497.pub2.
The incidence of pediatric Crohn's disease has been steadily increasing. In this population, the disease often presents with more extensive inflammation, a tendency toward a more aggressive course, and frequently requires early immunomodulation. Anti-tumor necrosis factor (TNF) antibodies work by neutralizing pro-inflammatory effectors, thus interrupting the inflammatory cascade. There is broad consensus that biologics are effective in achieving mucosal healing in Crohn's disease. Despite this, several important questions about anti-TNF therapy in children and adolescents remain unanswered. These include determining the optimal dosing regimen for both safety and durability, identifying the ideal timing for initiating anti-TNF treatment before irreversible bowel damage occurs, and deciding whether to use a top-down or step-up approach tailored to the individual patient's disease location, behavior, and other predictors of complicated outcomes.
To assess the efficacy and safety of TNF-alpha antagonists for induction of remission in children and adolescents with active Crohn's disease.
We searched the Cochrane Central Register of Controlled Trials (CENTRAL) in the Cochrane Library, PubMed, Embase (Elsevier), LILACS (Latin American and Caribbean Health Science Information database) (BIREME), and Science Citation Index Expanded and Conference Proceedings Citation Index-Science (Web of Science). We applied no language or document type restrictions. The last update of evidence was on 1 June 2024.
We included randomized controlled trials (RCTs), irrespective of publication type, publication status, and language, assessing the benefits and harms of TNF-alpha antagonist for induction of remission treatment for pediatric Crohn's disease.
Our critical outcomes were induction of clinical remission and incidence of serious adverse effects. Important outcomes were all-cause mortality and morbidity related to Crohn's disease, endoscopic remission, incidence of steroid withdrawal, proportion of participants in need of surgical intervention, loss of response to anti-TNF, and incidence of mild adverse events.
We assessed risk of bias using Cochrane's RoB 1 tool. The only included trial was at overall high risk of bias.
We used standard Cochrane methodology to perform this systematic review. We used the GRADE approach to assess the certainty of evidence per outcome.
Only one study fulfilled the inclusion criteria. The study was an open-label, multicenter RCT conducted in 12 hospitals in three European countries, and included 100 children (51 boys and 49 girls) newly diagnosed with moderate-to-severe Crohn's disease with a 52-week follow-up. Children were randomly assigned to first-line infiximab (FL-IFX) (n = 50) or conventional treatment (n = 50). The trial was at overall high risk of bias.
Clinical remission was achieved by 59% (24/41) in the FL-IFX group versus 34% (15/44) in the conventional-treatment group, therefore favoring FL-IFX (risk ratio [RR] 1.72, 95% confidence interval [CI] 1.06 to 2.79; low certainty evidence). Endoscopic remission was achieved by 59% (16/27) in the FL-IFX group versus 17% (5/30) in the conventional-treatment group, therefore favoring FL-IFX (RR 3.56, 95% CI 1.51 to 8.39; low certainty evidence). The included study did not assess all-cause morbidity or mortality related to Crohn's disease or incidence of serious or mild adverse events. No funding information was provided. This study is part of the TISKid study, which is in development and includes the same population with a planned follow-up of five years.
AUTHORS' CONCLUSIONS: There is limited evidence to support the use of anti-TNF therapy for induction of remission in pediatric Crohn's disease. Only one randomized clinical trial at high risk of bias suggests that FL-IFX may result in a slight increase in induction of clinical remission and endoscopic remission when compared to conventional treatment. The results of this trial need to be interpreted with caution. Several important questions remain regarding the optimal timing of anti-TNF therapy, the preference between step-up versus top-down strategies, and other related issues. Further RCTs are needed to achieve stronger evidence, address these questions, and provide clearer guidance. There is a need for larger randomized clinical trials following the SPIRIT and CONSORT statements, assessing the benefits and harms of using anti-TNF versus conventional therapy for pediatric Crohn's disease induction treatment.
This Cochrane review had no dedicated funding.
The intervention protocol was published on Cochrane Database of Systematic Reviews 2022, DOI: 10.1002/14651858.CD014497.
儿童克罗恩病的发病率一直在稳步上升。在这一人群中,该疾病通常表现为更广泛的炎症,病程往往更具侵袭性,且常常需要早期免疫调节。抗肿瘤坏死因子(TNF)抗体通过中和促炎效应因子发挥作用,从而中断炎症级联反应。人们普遍认为生物制剂在实现克罗恩病黏膜愈合方面是有效的。尽管如此,关于儿童和青少年抗TNF治疗仍有几个重要问题尚未得到解答。这些问题包括确定兼顾安全性和疗效持久性的最佳给药方案,确定在不可逆转的肠道损伤发生之前启动抗TNF治疗的理想时机,以及决定是采用根据个体患者的疾病部位、行为和其他复杂结局预测因素量身定制的自上而下还是逐步升级的治疗方法。
评估TNF-α拮抗剂对患有活动性克罗恩病的儿童和青少年诱导缓解的疗效和安全性。
我们检索了Cochrane图书馆中的Cochrane对照试验中央登记册(CENTRAL)、PubMed、Embase(爱思唯尔)、LILACS(拉丁美洲和加勒比健康科学信息数据库)(BIREME)以及科学引文索引扩展版和会议论文引文索引 - 科学版(科学网)。我们未设置语言或文献类型限制。证据的最后更新时间为2024年6月1日。
我们纳入了随机对照试验(RCT),无论其出版类型、出版状态和语言如何,评估TNF-α拮抗剂对儿童克罗恩病诱导缓解治疗的利弊。
我们的关键结局指标是临床缓解的诱导和严重不良反应的发生率。重要结局指标包括全因死亡率和与克罗恩病相关的发病率、内镜缓解、停用类固醇的发生率、需要手术干预的参与者比例、对抗TNF治疗反应的丧失以及轻度不良事件的发生率。
我们使用Cochrane的RoB 1工具评估偏倚风险。唯一纳入的试验总体偏倚风险较高。
我们采用标准的Cochrane方法进行这项系统评价。我们使用GRADE方法评估每个结局指标证据的确定性。
只有一项研究符合纳入标准。该研究是一项在三个欧洲国家的12家医院进行的开放标签、多中心RCT,纳入了100名新诊断为中度至重度克罗恩病的儿童(51名男孩和49名女孩),随访期为52周。儿童被随机分配至一线英夫利昔单抗(FL-IFX)组(n = 50)或传统治疗组(n = 50)。该试验总体偏倚风险较高。
FL-IFX组临床缓解率为59%(24/41),而传统治疗组为34%(15/44),因此FL-IFX更具优势(风险比[RR] 1.72,95%置信区间[CI] 1.06至2.79;低确定性证据)。FL-IFX组内镜缓解率为59%(16/27),而传统治疗组为17%(5/30),因此FL-IFX更具优势(RR 3.56,95% CI 1.51至8.39;低确定性证据)。纳入的研究未评估与克罗恩病相关的全因发病率或死亡率,也未评估严重或轻度不良事件的发生率。未提供资金信息。这项研究是TISKid研究的一部分,该研究正在进行中,纳入相同人群,计划随访五年。
支持在儿童克罗恩病中使用抗TNF治疗诱导缓解的证据有限。仅有一项偏倚风险较高的随机临床试验表明,与传统治疗相比,FL-IFX可能会使临床缓解和内镜缓解的诱导率略有增加。该试验结果需谨慎解读。关于抗TNF治疗的最佳时机、逐步升级与自上而下策略的选择以及其他相关问题,仍有几个重要问题有待解决。需要进一步的RCT以获得更有力的证据,解决这些问题,并提供更明确的指导。需要按照SPIRIT和CONSORT声明进行更大规模的随机临床试验,评估使用抗TNF与传统疗法对儿童克罗恩病诱导治疗的利弊。
本Cochrane综述无专项资金。
干预方案发表于《Cochrane系统评价数据库》2022年,DOI:10.1002/14651858.CD014497。
