Department of Pediatric Gastroenterology, Erasmus Medical Centre, Sophia Children's Hospital, Rotterdam, Netherlands.
Paediatric Gastroenterology, Centre for Immunobiology, Blizard Institute, Barts and the London School of Medicine, Queen Mary University of London, London, UK.
Lancet Child Adolesc Health. 2024 Jun;8(6):422-432. doi: 10.1016/S2352-4642(24)00078-6. Epub 2024 Apr 30.
Rare and severe adverse events can occur in children with inflammatory bowel disease (IBD), and the relationship with disease or drug treatment is often uncertain. We aimed to establish a method of reporting adverse events of interest in children with IBD, allowing for estimates of incidence rates with comparison between different regions, and, if possible, to compare with published data on rates of adverse events in children overall.
For this analysis, we used data from the Paediatric Inflammatory Bowel Disease Network for Safety, Efficacy and Treatment and Quality improvement of care (PIBD-SETQuality) Safety Registry, which collects data on multiple rare and severe adverse events in children younger than 19 years with IBD. Overall, the registry collected data on ten prespecified rare and severe adverse events in children with IBD, as established by a panel of paediatric IBD experts, via reports from paediatric gastroenterologists at participating hospitals between Nov 1, 2016, and March 31, 2023. Reporting physicians, who could only be paediatric gastroenterologists or IBD nurses reporting on behalf of paediatric gastroenterologists, were recruited through invitations sent to both national and international IBD networks and at conferences. Once per month, participating paediatric gastroenterologists received an email with an anonymous and unique link to an online survey asking them to report whether any of ten rare and severe adverse events had occurred in a patient in their paediatric-IBD population in the previous month. Prevalent or retrospective rare and severe adverse events were excluded, as were events occurring in children with an unconfirmed diagnosis of IBD or for whom inflammatory colitis was part of a monogenic immunodeficiency disorder. Duplicates and events that did not meet the definitions and criteria were excluded. Physicians could also report other, non-categorised adverse events if they considered them rare and severe. In case of no response, up to two reminders were sent for each per-month survey. Annual denominator data surveys were sent to obtain the total number of person-years for the estimation of incidence rates, which were calculated via Poisson regression models.
Responses were gathered from 220 paediatric gastroenterologists from 167 centres. 121 centres were in Europe, 23 centres were in North America, 17 centres were in Asia, and six centres were in Oceania. Combined, the total population with paediatric IBD consisted of an estimated 30 193 children with 114 528 person-years of follow-up. 451 adverse events were initially reported. After excluding and reorganising adverse events, 402 were eligible; 261 (65%) were categorised and 141 (35%) were non-categorised. The most frequently reported adverse events were venous-thromboembolic events (n=66), renal failure (n=43), opportunistic infections (n=42), and cancer (n=33). Haemophagocytic lymphohistiocytosis (n=4) and liver failure (n=3) were the least frequently reported adverse events. Incidence rates per 10 000 person-years were 5·50 (95% CI 4·25-6·97) for venous-thromboembolic events, 3·75 (2·74-4·99) for renal failure, 3·67 (2·67-4·89) for opportunistic infection, and 2·88 (2·01-3·98) for cancer. Of 66 venous-thromboembolic events, 31 (47%) involved cerebral venous sinus thrombosis at an incidence rate of 2·71 (95% CI 1·86-3·77).
The PIBD-SETQuality Safety Registry enabled us to identify incidence rates of rare and severe adverse events in children with IBD. Our findings can guide physicians and enhance awareness of the incidence of adverse events in children with IBD that are considered to be rare.
EU Horizon 2020 Research and Innovation Programme.
炎症性肠病(IBD)患儿可能会出现罕见且严重的不良事件,且这些不良事件与疾病或药物治疗的关系往往并不明确。本研究旨在建立一种报告 IBD 患儿不良事件的方法,以便在不同地区之间估计发生率,并尽可能与总体儿童不良事件发生率的已发表数据进行比较。
在这项分析中,我们使用了来自儿科炎症性肠病网络安全性、疗效和治疗以及护理质量改进(PIBD-SETQuality)安全性登记处的数据,该登记处收集了 19 岁以下 IBD 患儿多种罕见且严重不良事件的数据。总体而言,该登记处通过参与医院的儿科胃肠病学家报告,收集了由儿科 IBD 专家小组确定的 10 种罕见且严重不良事件的数据,报告时间为 2016 年 11 月 1 日至 2023 年 3 月 31 日。报告医师只能是儿科胃肠病学家或代表儿科胃肠病学家报告的 IBD 护士,他们是通过向国内外 IBD 网络和会议发出邀请招募而来的。每月一次,参与的儿科胃肠病学家会收到一封电子邮件,其中包含一个匿名且唯一的链接,可访问在线调查,要求他们报告前一个月其儿科 IBD 患者中是否发生了十种罕见且严重不良事件之一。排除现患或回顾性罕见且严重不良事件,以及未经确认的 IBD 诊断或炎症性结肠炎为单基因免疫缺陷疾病一部分的儿童。重复报告和不符合定义和标准的事件也被排除。如果医生认为是罕见且严重的其他非分类不良事件,也可以报告。如果没有回应,每个月的调查会发送两封提醒信。每年还会发送一次人数-年数据调查,以获得估计发病率所需的总人数,通过泊松回归模型计算发病率。
从 167 个中心的 220 名儿科胃肠病学家那里收集了回复。121 个中心位于欧洲,23 个中心位于北美,17 个中心位于亚洲,6 个中心位于大洋洲。总的来说,儿科 IBD 患者人群估计有 30193 名儿童,随访 114528 人年。最初报告了 451 起不良事件。在排除和重组不良事件后,有 402 起符合条件;其中 261 起(65%)进行了分类,141 起(35%)未分类。报告最多的不良事件是静脉血栓栓塞事件(n=66)、肾衰竭(n=43)、机会性感染(n=42)和癌症(n=33)。噬血细胞性淋巴组织细胞增生症(n=4)和肝衰竭(n=3)是报告最少的不良事件。每 10000 人年的发生率分别为静脉血栓栓塞事件 5.50(95%CI 4.25-6.97)、肾衰竭 3.75(2.74-4.99)、机会性感染 3.67(2.67-4.89)和癌症 2.88(2.01-3.98)。在 66 例静脉血栓栓塞事件中,31 例(47%)涉及脑静脉窦血栓形成,发生率为 2.71(95%CI 1.86-3.77)。
PIBD-SETQuality 安全性登记处使我们能够确定 IBD 患儿罕见且严重不良事件的发生率。我们的研究结果可以为医生提供指导,并提高对被认为罕见的 IBD 患儿不良事件发生率的认识。
欧盟地平线 2020 研究与创新计划。
