Ke Sun, Sicong Li, Bowen Zheng, Yanlei Zhu, Tongyue Wang, Mingfu Liang, Yue Yao, Kairan Zhang, Jizhong Zhang, Hongyong Li, Dongyang Han, Jishen Zheng, Brian Coventry, Longxing Cao, David Baker, Lei Liu, Peilong Lu
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引用次数: 0
Abstract
Abiotic D-proteins that selectively bind to natural L-proteins have gained significant biotechnological interest. However, the underlying structural principles governing such heterochiral protein-protein interactions remain largely unknown. In this study, we present the de novo design of D-proteins consisting of 50-65 residues, aiming to target specific surface regions of L-proteins or L-peptides. Our designer D-protein binders exhibit nanomolar affinity toward an artificial L-peptide, as well as two naturally occurring proteins of therapeutic significance: the D5 domain of human tropomyosin receptor kinase A (TrkA) and human interleukin-6 (IL-6). Notably, these D-protein binders demonstrate high enantiomeric specificity and target specificity. In cell-based experiments, designer D-protein binders effectively inhibited the downstream signaling of TrkA and IL-6 with high potency. Moreover, these binders exhibited remarkable thermal stability and resistance to protease degradation. Crystal structure of the designed heterochiral D-protein-L-peptide complex, obtained at a resolution of 2.0 Å, closely resembled the design model, indicating that the computational method employed is highly accurate. Furthermore, the crystal structure provides valuable information regarding the interactions between helical L-peptides and D-proteins, particularly elucidating a novel mode of heterochiral helix-helix interactions. Leveraging the design of D-proteins specifically targeting L-peptides or L-proteins opens up avenues for systematic exploration of the mirror-image protein universe, paving the way for a diverse range of applications.
选择性地与天然 L 蛋白结合的非生物 D 蛋白已引起生物技术的极大兴趣。然而,制约这种异手性蛋白-蛋白相互作用的基本结构原理在很大程度上仍不为人所知。在本研究中,我们从头开始设计了由 50-65 个残基组成的 D 蛋白,旨在靶向 L 蛋白或 L 肽的特定表面区域。我们设计的D蛋白结合剂对人工L肽以及两种具有治疗意义的天然蛋白(人肌钙蛋白受体激酶A(TrkA)的D5结构域和人白细胞介素-6(IL-6))具有纳摩尔级的亲和力。值得注意的是,这些 D 蛋白结合剂具有很高的对映体特异性和靶向特异性。在基于细胞的实验中,设计的 D 蛋白结合剂以高效力有效抑制了 TrkA 和 IL-6 的下游信号传导。此外,这些结合剂还具有显著的热稳定性和抗蛋白酶降解性。所设计的异手性 D 蛋白-L 肽复合物的晶体结构分辨率为 2.0 Å,与设计模型非常相似,表明所采用的计算方法非常精确。此外,该晶体结构还为螺旋 L 肽和 D 蛋白之间的相互作用提供了宝贵的信息,特别是阐明了一种新型的异螺旋-螺旋相互作用模式。利用专门针对 L 肽或 L 蛋白的 D 蛋白设计为系统探索镜像蛋白质宇宙开辟了途径,为各种应用铺平了道路。
期刊介绍:
Cell Research (CR) is an international journal published by Springer Nature in partnership with the Center for Excellence in Molecular Cell Science, Chinese Academy of Sciences (CAS). It focuses on publishing original research articles and reviews in various areas of life sciences, particularly those related to molecular and cell biology. The journal covers a broad range of topics including cell growth, differentiation, and apoptosis; signal transduction; stem cell biology and development; chromatin, epigenetics, and transcription; RNA biology; structural and molecular biology; cancer biology and metabolism; immunity and molecular pathogenesis; molecular and cellular neuroscience; plant molecular and cell biology; and omics, system biology, and synthetic biology. CR is recognized as China's best international journal in life sciences and is part of Springer Nature's prestigious family of Molecular Cell Biology journals.