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古塞库单抗与司库奇尤单抗对银屑病生物标志物的差异药效学效应与长期疗效相关:一项ECLIPSE子研究

Differential Pharmacodynamic Effects on Psoriatic Biomarkers by Guselkumab Versus Secukinumab Correlate with Long-Term Efficacy: An ECLIPSE Substudy.

作者信息

Blauvelt Andrew, Chen Yanqing, Branigan Patrick J, Liu Xuejun, DePrimo Samuel, Keyes Brice E, Leung Monica, Fakharzadeh Steven, Yang Ya-Wen, Muñoz-Elías Ernesto J, Krueger James G, Langley Richard G

机构信息

Blauvelt Consulting LLC, Lake Oswego, Oregon, USA.

Janssen Research & Development, LLC, San Diego, California, USA.

出版信息

JID Innov. 2024 Jun 26;4(5):100297. doi: 10.1016/j.xjidi.2024.100297. eCollection 2024 Sep.

DOI:10.1016/j.xjidi.2024.100297
PMID:39224116
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11367549/
Abstract

IL-23 is a cytokine produced by myeloid cells that drives the T helper 17 pathway and plays an essential role in the pathophysiology of plaque psoriasis. IL-23 activation initiates a cascade of cytokines subsequently inducing the expression of many psoriasis-related proteins. This study aimed to better understand the underlying mechanisms driving the differences between IL-23 and IL-17A blockade in patients with psoriasis and their implications for durability of clinical responses. Serum and/or skin biopsies were isolated from patients treated with guselkumab or secukinumab for evaluation of potential biomarkers of pharmacodynamic response to treatment. Guselkumab treatment led to significantly greater reductions of IL-17F and IL-22 serum levels than treatment with secukinumab at weeks 24 and 48, demonstrating sustained regulation of the IL-23/T helper 17 pathway. Analyses of proteomic and transcriptomic profiles of patient sera and skin biopsies demonstrated differential regulation of proteins involved in chemokine, TNF, and relevant immune signaling pathways to a greater degree with guselkumab than with secukinumab treatment. These data provide insights into the differences between the mechanisms and impact of IL-23 and IL-17A blockade in psoriasis, with implications for efficacy observations and treatment paradigms. Trial Registration: The original study was registered at ClinicalTrials.gov (NCT03090100).

摘要

白细胞介素-23(IL-23)是一种由髓样细胞产生的细胞因子,它驱动辅助性T细胞17(Th17)通路,在斑块状银屑病的病理生理学中起重要作用。IL-23激活引发一系列细胞因子,随后诱导许多银屑病相关蛋白的表达。本研究旨在更好地理解银屑病患者中IL-23和IL-17A阻断差异的潜在机制及其对临床反应持久性的影响。从接受古塞库单抗或司库奇尤单抗治疗的患者中分离血清和/或皮肤活检组织,以评估治疗药效学反应的潜在生物标志物。在第24周和第48周时,与司库奇尤单抗治疗相比,古塞库单抗治疗导致IL-17F和IL-22血清水平显著降低,表明对IL-23/Th17通路的持续调节。对患者血清和皮肤活检组织的蛋白质组学和转录组学谱分析表明,与司库奇尤单抗治疗相比,古塞库单抗治疗在更大程度上对趋化因子、肿瘤坏死因子(TNF)和相关免疫信号通路中涉及的蛋白质进行了差异调节。这些数据为银屑病中IL-23和IL-17A阻断的机制和影响差异提供了见解,对疗效观察和治疗模式具有启示意义。试验注册:原始研究在ClinicalTrials.gov(NCT03090100)注册。

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