Interleukin-17 Inhibitors and Early Major Adverse Cardiovascular Events.

IF 11 1区医学 Q1 DERMATOLOGY

JAMA dermatology Pub Date : 2025-09-03 DOI:10.1001/jamadermatol.2025.2972

Maxime Raby, Frederic Balusson, Emmanuel Oger, Marion Gundelwein, Alain Dupuy, Florence Poizeau

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引用次数: 0

Abstract

Importance: The cardiovascular impact of biologics used in psoriasis is not fully understood. Several studies have suggested that the inhibition of the T-helper 17 cell pathway could lead to the destabilization of atherosclerotic plaques, leading to major adverse cardiovascular events (MACEs).

Objective: To assess whether the initiation of interleukin (IL)-17(R)A inhibitors triggers MACEs.

Design, setting, and participants: In this case-time-control study using the French National Health Insurance database, all individuals who received IL-17(R)A inhibitors (secukinumab, ixekizumab, and brodalumab) from 2016 to 2021, were included and classified according to their cardiovascular risk level. The risk period was defined as the 6 months before the MACE, and the reference period as the 6 months before the risk period. The same design for patients who received tumor necrosis factor (TNF)-α inhibitors (adalimumab or etanercept) for similar indications (psoriasis, psoriatic arthritis, ankylosing spondylitis, or juvenile arthritis), as an active comparator. The data analysis was conducted between April 2023 and August 2024.

Exposure: The initiation of the biologic was screened in both periods.

Main outcomes and measures: The odds ratios (ORs) for the risk of MACEs were assessed following the initiation of IL-17(R)A inhibitors and TNF-α inhibitors independently. Subsequently, the OR for the risk of MACE associated with IL-17(R)A inhibitors was estimated using TNF-α inhibitors as the comparator.

Results: Among the 34 241 individuals who received an IL-17(R)A inhibitor, 381 MACEs were analyzed, including 176 acute coronary syndromes and 84 ischemic strokes in the main analysis. Initiation of IL-17(R)A inhibitors was not significantly associated with MACEs (OR, 1.25 [95% CI, 0.75-2.08] vs TNF-α inhibitor initiation and MACEs: OR, 0.90 [95% CI, 0.65-1.24]). Overall, the initiation of an IL-17(R)A inhibitor was not significantly associated with MACEs in the following 6 months, using TNF-α inhibitor as a comparator (OR, 1.40 [95% CI, 0.77-2.54]), regardless of the individual cardiovascular risk (P for homogeneity = .29). The definition of MACE was broadened in a first sensitivity analysis, and the risk period was shortened to 3 months in a second sensitivity analysis. The results did not change.

Conclusions: In this case-time-control study based on a national insurance database, there was no evidence of a significant association between MACEs and the initiation of IL-17(R)A inhibitors, regardless of the individual cardiovascular risk of the patient. However, a modest risk increase cannot be entirely excluded.

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白细胞介素-17抑制剂与早期主要不良心血管事件。

重要性：银屑病生物制剂对心血管的影响尚不完全清楚。一些研究表明，t -辅助性17细胞通路的抑制可能导致动脉粥样硬化斑块的不稳定，导致主要的不良心血管事件（mace）。目的：评估启动白细胞介素(IL)-17(R)A抑制剂是否触发mace。设计、环境和参与者：在这项使用法国国家健康保险数据库的病例-时间对照研究中，所有在2016年至2021年接受IL-17(R)A抑制剂（secukinumab、ixekizumab和brodalumab）治疗的个体都被纳入研究，并根据其心血管风险水平进行分类。风险期定义为MACE发生前6个月，参照期定义为风险期发生前6个月。同样的设计也适用于接受肿瘤坏死因子(TNF)-α抑制剂（阿达木单抗或依那西普）治疗类似适应症（银屑病、银屑病关节炎、强直性脊柱炎或幼年关节炎）的患者，作为活性比较。数据分析在2023年4月至2024年8月期间进行。暴露：在两个时期筛选生物制剂的起始。主要结局和指标：分别评估IL-17(R)A抑制剂和TNF-α抑制剂启动后mace风险的比值比（ORs）。随后，以TNF-α抑制剂为比较物，估计与IL-17(R)A抑制剂相关的MACE风险的OR。结果：在34 241例接受IL-17(R)A抑制剂治疗的患者中，分析了381例mace，其中176例为急性冠状动脉综合征，84例为缺血性卒中。IL-17(R)A抑制剂的启动与mace无显著相关性（OR, 1.25 [95% CI, 0.75-2.08]，而TNF-α抑制剂的启动和mace: OR， 0.90 [95% CI, 0.65-1.24]）。总体而言，无论个体心血管风险如何，以TNF-α抑制剂为比较指标，IL-17(R)A抑制剂的起始与随后6个月的mace无显著相关性（OR, 1.40 [95% CI, 0.77-2.54]）（同质性P = 0.29）。第一次敏感性分析拓宽了MACE的定义，第二次敏感性分析将风险期缩短至3个月。结果没有改变。结论：在这项基于国家保险数据库的病例-时间-对照研究中，没有证据表明mace与IL-17(R) a抑制剂的启动之间存在显著关联，无论患者的个体心血管风险如何。然而，不能完全排除适度的风险增加。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

JAMA dermatology DERMATOLOGY-

CiteScore

14.10

自引率

5.50%

发文量

300

期刊介绍： JAMA Dermatology is an international peer-reviewed journal that has been in continuous publication since 1882. It began publication by the American Medical Association in 1920 as Archives of Dermatology and Syphilology. The journal publishes material that helps in the development and testing of the effectiveness of diagnosis and treatment in medical and surgical dermatology, pediatric and geriatric dermatology, and oncologic and aesthetic dermatologic surgery. JAMA Dermatology is a member of the JAMA Network, a consortium of peer-reviewed, general medical and specialty publications. It is published online weekly, every Wednesday, and in 12 print/online issues a year. The mission of the journal is to elevate the art and science of health and diseases of skin, hair, nails, and mucous membranes, and their treatment, with the aim of enabling dermatologists to deliver evidence-based, high-value medical and surgical dermatologic care. The journal publishes a broad range of innovative studies and trials that shift research and clinical practice paradigms, expand the understanding of the burden of dermatologic diseases and key outcomes, improve the practice of dermatology, and ensure equitable care to all patients. It also features research and opinion examining ethical, moral, socioeconomic, educational, and political issues relevant to dermatologists, aiming to enable ongoing improvement to the workforce, scope of practice, and the training of future dermatologists. JAMA Dermatology aims to be a leader in developing initiatives to improve diversity, equity, and inclusion within the specialty and within dermatology medical publishing.