Proline-Mediated Enhancement in Evolvability of Disulfide-Rich Peptides for Discovering Protein Binders.

IF 14.4 1区化学 Q1 CHEMISTRY, MULTIDISCIPLINARY

Journal of the American Chemical Society Pub Date : 2025-07-02 DOI:10.1021/jacs.5c07075

Hongtan Liu,Lulu Song,Xiaoting Meng,Jinjing Li,Shihui Fan,Huilei Dong,Xiaoran Wang,Maolin Li,Haipeng Yu,Yu-Hsuan Tsai,Yizhen Yin,Chuanliu Wu

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引用次数: 0

Abstract

Disulfide-rich peptides (DRPs), particularly those featuring the inhibitor cystine knot (ICK) motif, represent promising scaffolds for developing next-generation protein modulators and therapeutic agents due to their remarkable stability and specificity. However, their inherent structural integrity and lack of structural plasticity significantly limit their evolvability, creating a fundamental bottleneck in engineering novel functionalities. To address this challenge, we developed a novel proline scanning strategy aimed at enhancing the evolvability of the ICK scaffolds. This strategy leverages the proline-mediated structural decoupling between scaffold and nonscaffold residues in DRPs to promote their evolvability. By strategically incorporating prolines as pre-encoded scaffold residues, we engineered ICK variants with significantly improved foldability and tolerance to sequence variations. This advancement enabled the construction of diverse peptide libraries suitable for screening platforms, including mRNA and phage display. Utilizing this approach, we successfully identified DRPs exhibiting low-nanomolar affinity to clinically important targets, such as TROP2 and 4-1BB. Structural characterization revealed that these evolved DRPs adopted unique three-dimensional structures stabilized by up to four disulfide bonds, demonstrating both high oxidative folding efficiency and enhanced evolvability due to proline incorporation. To evaluate their therapeutic potential, we developed a DRP-based chimeric antigen receptor (CAR) targeting TROP2. The DRP-based CAR T cells exhibited potency comparable to conventional single-chain variable fragment (scFv)-based CAR T cells but with a notably improved safety profile. Overall, our work establishes a robust framework for expanding the functional versatility of DRP scaffolds, facilitating the discovery and development of structurally diverse and functional DRPs for broad applications in therapeutics and drug development.

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脯氨酸介导的富二硫肽的进化能力增强用于发现蛋白质结合物。

富二硫肽（DRPs），特别是那些具有抑制剂胱氨酸结（ICK）基序的肽，由于其显著的稳定性和特异性，是开发下一代蛋白质调节剂和治疗剂的有前途的支架。然而，它们固有的结构完整性和结构可塑性的缺乏极大地限制了它们的可进化性，成为工程新功能的根本瓶颈。为了应对这一挑战，我们开发了一种新的脯氨酸扫描策略，旨在增强ICK支架的可进化性。该策略利用脯氨酸介导的DRPs中支架和非支架残基之间的结构解耦来促进它们的可进化性。通过战略性地将脯氨酸作为预编码的支架残基，我们设计了ICK变体，显著提高了可折叠性和对序列变化的耐受性。这一进展使得构建适合筛选平台的多种肽库，包括mRNA和噬菌体展示。利用这种方法，我们成功地鉴定出对临床上重要靶点（如TROP2和4-1BB）具有低纳摩尔亲和力的DRPs。结构表征表明，这些进化的DRPs采用独特的三维结构，由多达四个二硫键稳定，显示出高的氧化折叠效率和由于脯氨酸的加入而增强的进化性。为了评估它们的治疗潜力，我们开发了一种基于drp的靶向TROP2的嵌合抗原受体（CAR）。基于drp的CAR - T细胞表现出与传统的基于单链可变片段（scFv）的CAR - T细胞相当的效力，但安全性显著提高。总的来说，我们的工作为扩大DRP支架的功能多样性建立了一个强大的框架，促进了结构多样化和功能丰富的DRP的发现和开发，以广泛应用于治疗和药物开发。

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

Journal of the American Chemical Society 化学-化学综合

CiteScore

24.40

自引率

6.00%

发文量

2398

审稿时长

1.6 months

期刊介绍： The flagship journal of the American Chemical Society, known as the Journal of the American Chemical Society (JACS), has been a prestigious publication since its establishment in 1879. It holds a preeminent position in the field of chemistry and related interdisciplinary sciences. JACS is committed to disseminating cutting-edge research papers, covering a wide range of topics, and encompasses approximately 19,000 pages of Articles, Communications, and Perspectives annually. With a weekly publication frequency, JACS plays a vital role in advancing the field of chemistry by providing essential research.