Structural Basis for p19 Targeting by Anti–IL-23 Biologics: Correlations with Short- and Long-Term Efficacy in Psoriasis

Stefano G. Daniele , Sherif A. Eldirany , Giovanni Damiani , Minh Ho , Christopher G. Bunick
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Abstract

IL-23 is central to psoriasis pathogenesis. Biologics targeting IL-23 are important therapies against psoriasis. IL-23 inhibitors risankizumab, tildrakizumab, and guselkumab bind the IL-23 p19 subunit, whereas ustekinumab binds p40; however, the structural composition of the IL-23–binding epitopes and how these molecular properties relate to clinical efficacy are not known. Utilizing epitope data derived from hydrogen-deuterium exchange or crystallographic experiments, we mapped inhibitor epitope locations, hydrophobicity, and surface charge onto the IL-23 surface. Molecular properties of each inhibitor epitope, including solvent-accessible surface area, were correlated to binding affinity, kinetic values, and clinical efficacy scores for plaque psoriasis through linear regression analysis. Each IL-23 inhibitor binds an epitope with a unique size, composition, and location except for a 10-residue overlap region outside of the IL-23 receptor epitope. We observed strong correlations between epitope surface area and KD and koff but not kon. Epitope surface area, KD, and koff were further associated with short-term (10–16 weeks) and long-term (44–60 weeks) clinical efficacy according to PASI-90 responses, with risankizumab demonstrating highest efficacy among IL-23 biologics. In contrast, kon, epitope hydrophobicity, polarity, and charge content did not correlate with efficacy. These data exemplify how molecular principles of medications within a therapeutic class can explain their differential clinical responses.

Abstract Image

抗IL-23生物制剂不同p19靶向作用的结构基础:与银屑病短期和长期临床疗效的相关性
IL-23 是银屑病发病机制的核心。针对IL-23的生物制剂是治疗银屑病的重要疗法。IL-23抑制剂risankizumab、tildrakizumab和guselkumab与IL-23 p19亚基结合,而ustekinumab与p40结合;然而,IL-23结合表位的结构组成以及这些分子特性与临床疗效的关系尚不清楚。利用氢氘交换或晶体学实验得出的表位数据,我们将抑制剂表位的位置、疏水性和表面电荷绘制到了IL-23表面。通过线性回归分析,每个抑制剂表位的分子特性(包括可溶解表面积)都与结合亲和力、动力学值和斑块型银屑病的临床疗效评分相关联。除了 IL-23 受体表位外的 10 个残基重叠区外,每种 IL-23 抑制剂结合的表位都有独特的大小、组成和位置。我们观察到表位表面积与 KD 和 koff 之间有很强的相关性,但与 kon 没有相关性。根据 PASI-90 反应,表位表面积、KD 和 koff 与短期(10-16 周)和长期(44-60 周)临床疗效进一步相关,其中利桑珠单抗在 IL-23 生物制剂中疗效最高。相比之下,kon、表位疏水性、极性和电荷含量与疗效无关。这些数据说明了治疗类药物的分子原理如何解释其不同的临床反应。
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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