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接受五种不同白细胞介素抑制剂治疗的银屑病患者新发炎症性肠病的风险:一项系统评价和荟萃分析

Risk of new-onset inflammatory bowel disease in psoriasis patients treated with five different interleukin inhibitors: a systematic review and meta-analysis.

作者信息

Zhang Jia-Xin, Li Wen-Wei, Huang Long-Zhuan, Lai Sha, Qiu Zhi-Kun

机构信息

Key Specialty of Clinical Pharmacy, The First Affiliated Hospital of Guangdong Pharmaceutical University, Guangzhou, China.

出版信息

Front Immunol. 2025 Jun 4;16:1594998. doi: 10.3389/fimmu.2025.1594998. eCollection 2025.

DOI:10.3389/fimmu.2025.1594998
PMID:40534876
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12174387/
Abstract

BACKGROUND

Interleukin inhibitors represent a standard therapeutic approach for psoriasis. However, there is still debate about the risk of new-onset inflammatory bowel disease (IBD) in psoriasis patients following interleukin inhibitor treatment. This systematic review and meta-analysis aims to evaluate the risk of new-onset IBD in psoriasis patients treated with five interleukin inhibitors (Bimekizumab, Ixekizumab, Secukinumab, Brodalumab, and Ustekinumab), providing insights to inform clinical decision-making.

METHOD

This study was registered in the PROSPERO with registration number of CRD42024608423. The databases PubMed, Embase, Cochrane Library, and Web of Science were comprehensively searched for observational studies published as full-length papers in English. The Mantel-Haenszel method with a fixed-effects model and risk difference was used to compare the risk of new-onset IBD between experimental groups (using interleukin inhibitors) and the control groups (using placebo or non-interleukin inhibitors). Sensitivity analysis was performed using the leave-one-out method for the meta-analysis. Additionally, considering the potential for underdiagnosis of IBD, a meta-analysis of the risk of diarrhea was conducted.

RESULT

This study included 17 articles covering 21 Randomized Controlled Trials(RCTs). A total of 22 new-onset IBD cases were reported in the experimental groups, with 3, 14, 4, 1, and 0 cases in the Bimekizumab, Ixekizumab, Secukinumab, Brodalumab, and Ustekinumab group, respectively. The control group only reported 1 case of new-onset IBD. No significant difference in the risk of new-onset IBD was found between these experimental groups and control groups. Based on the fixed-effects model, the pooled risk difference for Ixekizumab group was MH RD 0.0027 (95% CI 0.0001-0.0054, I² = 0%, P = 0.04). Sensitivity analysis indicated that the data was stable. Regarding diarrhea, a total of 95 cases were reported in the experimental groups, compared to 50 cases in the control groups. The experimental groups of Bimekizumab, Secukinumab, and Brodalumab reported 49, 45, and 1 case of diarrhea, respectively, while their control groups reported 11, 39, and 0 cases, respectively. Based on the fixed-effects model, compared to the control groups, there were no significant differences in the risk of diarrhea among psoriasis patients treated with these three interleukin inhibitors, and sensitivity analysis demonstrated good data robustness. Additionally, no cases of diarrhea were reported in the Ixekizumab group and Ustekinumab group.

CONCLUSIONS

There is insufficient evidence to confirm that Ustekinumab, Bimekizumab, Secukinumab, and Brodalumab significantly increase the risk of new-onset IBD. However, compared to the control group, Ixekizumab was significantly associated with an increased risk of new-onset IBD in psoriasis patients. Psoriasis patients receiving Ixekizumab treatment should remain vigilant for gastrointestinal symptoms, particularly in high-risk patients, to identify and manage potential IBD early. Additionally, compared to the control group, no significant difference was observed in the risk of diarrhea as an adverse event among patients treated with Bimekizumab, Secukinumab, and Brodalumab.

SYSTEMATIC REVIEW REGISTRATION

https://www.crd.york.ac.uk/PROSPERO/view/CRD42024608423, identifier CRD42024608423.

摘要

背景

白细胞介素抑制剂是银屑病的标准治疗方法。然而,对于银屑病患者在接受白细胞介素抑制剂治疗后新发炎症性肠病(IBD)的风险仍存在争议。本系统评价和荟萃分析旨在评估接受五种白细胞介素抑制剂(比美吉珠单抗、司库奇尤单抗、依奇珠单抗、布罗达单抗和乌司奴单抗)治疗的银屑病患者新发IBD的风险,为临床决策提供参考依据。

方法

本研究在国际前瞻性系统评价注册库(PROSPERO)注册,注册号为CRD42024608423。全面检索了PubMed、Embase、Cochrane图书馆和Web of Science数据库,以查找以英文全文发表的观察性研究。采用固定效应模型的Mantel-Haenszel方法和风险差值来比较实验组(使用白细胞介素抑制剂)和对照组(使用安慰剂或非白细胞介素抑制剂)中新发IBD的风险。采用逐一剔除法对荟萃分析进行敏感性分析。此外,考虑到IBD可能存在诊断不足的情况,对腹泻风险进行了荟萃分析。

结果

本研究纳入了17篇文章,涵盖21项随机对照试验(RCT)。实验组共报告22例新发IBD病例,其中比美吉珠单抗组3例、依奇珠单抗组14例、司库奇尤单抗组4例、布罗达单抗组1例、乌司奴单抗组0例。对照组仅报告1例新发IBD。这些实验组与对照组之间新发IBD的风险未发现显著差异。基于固定效应模型,依奇珠单抗组的合并风险差值为MH RD 0.0027(95%CI 0.0001 - 0.0054,I² = 0%,P = 0.04)。敏感性分析表明数据稳定。关于腹泻,实验组共报告95例,对照组报告50例。比美吉珠单抗组、司库奇尤单抗组和布罗达单抗组的实验组分别报告49例、45例和1例腹泻,而其对照组分别报告11例、39例和0例。基于固定效应模型,与对照组相比,接受这三种白细胞介素抑制剂治疗的银屑病患者腹泻风险无显著差异,敏感性分析显示数据稳健性良好。此外,依奇珠单抗组和乌司奴单抗组未报告腹泻病例。

结论

没有足够的证据证实乌司奴单抗、比美吉珠单抗、司库奇尤单抗和布罗达单抗会显著增加新发IBD的风险。然而,与对照组相比,依奇珠单抗与银屑病患者新发IBD风险增加显著相关。接受依奇珠单抗治疗的银屑病患者应警惕胃肠道症状,尤其是高危患者,以便早期识别和管理潜在的IBD。此外,与对照组相比,接受比美吉珠单抗、司库奇尤单抗和布罗达单抗治疗的患者发生腹泻作为不良事件的风险未观察到显著差异。

系统评价注册

https://www.crd.york.ac.uk/PROSPERO/view/CRD42024608423,标识符CRD42024608423。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1d3a/12174387/605629609948/fimmu-16-1594998-g009.jpg
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