Molecular modeling and rational design of disulfide-stapled self-inhibitory peptides to target IL-17A/IL-17RA interaction

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2023-07-06 DOI:10.1002/jmr.3045

Weihua Huang, Yang Zhou, Chunhua Pan, Xin Zhang, Huijun Zhao, Lili Shen

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Abstract

Interleukin-17A (IL-17A) is a pro-inflammatory cytokine implicated in diverse autoimmune and inflammatory disorders such as psoriasis and Kawasaki disease. Mature IL-17A is a homodimer that binds to the extracellular type-III fibronectin D1:D2-dual domain of its cognate IL-17 receptor A (IL-17RA). In this study, we systematically examined the structural basis, thermodynamics property, and dynamics behavior of IL-17RA/IL-17A interaction and computationally identified two continuous hotspot regions separately from different monomers of IL-17A homodimer that contribute significantly to the interaction, namely I-shaped and U-shaped segments, thus rendered as a peptide-mediated protein–protein interaction (PmPPI). Self-inhibitory peptides (SIPs) are derived from the two segments to disrupt IL-17RA/IL-17A interaction by competitively rebinding to the IL-17A-binding pocket on IL-17RA surface, which, however, only have a weak affinity and low specificity for IL-17RA due to lack of the context support of intact IL-17A protein, thus exhibiting a large flexibility and intrinsic disorder when splitting from the protein context and incurring a considerable entropy penalty when rebinding to IL-17RA. The U-shaped segment is further extended, mutated and stapled by a disulfide bridge across its two strands to obtain a number of double-stranded cyclic SIPs, which are partially ordered and conformationally similar to their native status at IL-17RA/IL-17A complex interface. Experimental fluorescence polarization assays substantiate that the stapling can moderately or considerably improve the binding affinity of U-shaped segment-derived peptides by 2–5-fold. In addition, computational structural modeling also reveals that the stapled peptides can bind in a similar mode with the native crystal conformation of U-shaped segment in IL-17RA pocket, where the disulfide bridge is out of the pocket for avoiding intervene of the peptide binding.

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靶向IL-17A/IL-17RA相互作用的二硫自抑制肽的分子建模和合理设计

白细胞介素- 17a (IL-17A)是一种促炎细胞因子，与多种自身免疫性和炎症性疾病(如牛皮癣和川崎病)有关。成熟的IL-17A是一种同二聚体，结合其同源IL-17受体a (IL-17RA)的细胞外iii型纤维连接蛋白D1: d2双结构域。在本研究中，我们系统地研究了IL-17RA/IL-17A相互作用的结构基础、热力学性质和动力学行为，并分别从IL-17A同型二聚体的不同单体中计算出两个对相互作用有重要贡献的连续热点区域，即i型和u型区段，从而表征为肽介导的蛋白-蛋白相互作用(PmPPI)。自抑制肽(SIPs)是由这两个片段衍生而来，通过竞争性地重新结合IL-17RA表面上的IL-17A结合口袋来破坏IL-17RA/IL-17A的相互作用，但由于缺乏完整IL-17A蛋白的上下文支持，SIPs对IL-17RA只有较弱的亲和力和较低的特异性，因此在脱离蛋白质上下文时表现出很大的灵活性和内在的无序性，在重新结合IL-17RA时产生相当大的熵惩罚。u形片段被进一步延长、突变并通过其两条链上的二硫桥接而成，以获得一些双链环状SIPs，这些SIPs部分有序，构象与IL-17RA/IL-17A复合物界面上的天然状态相似。实验荧光偏振分析证实，钉接可以适度或显著提高u型片段衍生肽的结合亲和力，提高2 - 5倍。此外，计算结构模型还显示，钉接肽可以以类似于IL-17RA口袋中u型片段的天然晶体构象结合，其中二硫桥不在口袋中，以避免干预肽的结合。

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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