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比较中重度斑块状银屑病生物制剂与口服治疗的安全性和获益-风险特征:临床试验数据的网络荟萃分析。

Comparative safety and benefit-risk profile of biologics and oral treatment for moderate-to-severe plaque psoriasis: A network meta-analysis of clinical trial data.

机构信息

Sunnybrook Health Sciences Centre, University of Toronto, Toronto, Canada.

Analysis Group, Inc, Los Angeles, California.

出版信息

J Am Acad Dermatol. 2021 Sep;85(3):572-581. doi: 10.1016/j.jaad.2021.02.057. Epub 2021 Feb 22.

DOI:10.1016/j.jaad.2021.02.057
PMID:33631216
Abstract

BACKGROUND

The comparative safety and benefit-risk profiles of moderate-to-severe psoriasis treatment have not been well studied.

OBJECTIVE

To compare the short-term (12-16 weeks) and long-term (48-56 weeks) safety and benefit-risk profiles of moderate-to-severe psoriasis treatments.

METHODS

A systematic literature review of phase II-IV randomized controlled trials of moderate-to-severe psoriasis treatments was conducted (cutoff: July 1, 2020). Any adverse events (AEs), any serious AEs, and AEs leading to treatment discontinuation were compared using Bayesian network meta-analyses (NMAs).

RESULTS

Fifty-two and 7, respectively, randomized controlled trials were included in the short- and long-term NMAs, respectively. In the short-term NMA, the rates of any AEs were the lowest for tildrakizumab (posterior median: 46.0%), certolizumab (46.2%), and etanercept (49.1%). The rates of any serious AE were the lowest for certolizumab (0.8%), risankizumab (1.2%), and etanercept (1.6%). The rates of AEs leading to treatment discontinuation were the lowest for risankizumab (0.5%), tildrakizumab (1.0%), and guselkumab (1.5%). In the long-term NMA, risankizumab had the lowest rates of all 3 outcomes (67.5%, 4.4%, and 1.0%, respectively) and the most favorable benefit-risk profile.

LIMITATIONS

The results may not be generalizable to real-world populations.

CONCLUSIONS

Anti-interleukin 23 agents were associated with low rates of safety events. Risankizumab had the most favorable benefit-risk profile in the long term.

摘要

背景

中重度银屑病治疗的相对安全性和获益风险特征尚未得到充分研究。

目的

比较中重度银屑病治疗的短期(12-16 周)和长期(48-56 周)安全性和获益风险特征。

方法

对中重度银屑病治疗的 II-IV 期随机对照试验进行了系统的文献回顾(截止日期:2020 年 7 月 1 日)。使用贝叶斯网络荟萃分析(NMA)比较任何不良事件(AE)、任何严重 AE 和导致治疗中断的 AE。

结果

分别纳入了 52 项和 7 项短期和长期 NMA 的随机对照试验。在短期 NMA 中,阿特朱单抗(后验中位数:46.0%)、certolizumab(46.2%)和依那西普(49.1%)的 AE 发生率最低。certolizumab(0.8%)、risankizumab(1.2%)和依那西普(1.6%)的严重 AE 发生率最低。risankizumab(0.5%)、阿特朱单抗(1.0%)和古塞库单抗(1.5%)的治疗中断 AE 发生率最低。在长期 NMA 中,risankizumab 这 3 项结局的发生率均最低(分别为 67.5%、4.4%和 1.0%),且获益风险比最有利。

局限性

结果可能不适用于真实世界人群。

结论

抗白细胞介素 23 制剂与低安全性事件发生率相关。risankizumab 在长期治疗中具有最有利的获益风险比。

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