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科学家实现SARS-CoV-2小蛋白抑制剂的从头设计
作者:小柯机器人 发布时间:2020/9/12 22:30:21

美国华盛顿大学David Baker课题组从头设计出SARS-CoV-2的小蛋白抑制剂。相关论文于2020年9月9日在线发表于国际学术期刊《科学》。

据研究人员介绍,靶向SARS-CoV-2突刺蛋白和人类ACE2受体之间的相互作用是一种有前途的治疗策略。
 
研究人员使用两种从头设计方法来设计抑制剂。计算机生成的支架要么围绕与突刺受体结合域(RBD)相互作用的ACE2螺旋构建,要么依赖RBD对接来鉴定新的结合模式,并且这些氨基酸序列设计用于优化靶标结合、折叠和稳定性。
 
十个设计以100pM至10nM的亲和力结合RBD,并阻断了IC 50值为24pM至35nM的Vero E6细胞的SARS-CoV-2感染;最有效是56和64个残基的蛋白(IC 50?0.16ng/ml)。这些微型粘合分子与SARS-CoV-2突刺胞外域三聚体结合所有三个RBD的冷冻电镜结构与计算模型几乎相同。这些超稳定的迷你粘合分子为SARS-CoV-2治疗提供了起点。
 
附:英文原文
 
Title: De novo design of picomolar SARS-CoV-2 miniprotein inhibitors

Author: Longxing Cao, Inna Goreshnik, Brian Coventry, James Brett Case, Lauren Miller, Lisa Kozodoy, Rita E. Chen, Lauren Carter, Alexandra C. Walls, Young-Jun Park, Eva-Maria Strauch, Lance Stewart, Michael S. Diamond, David Veesler, David Baker

Issue&Volume: 2020/09/09

Abstract: Abstract Targeting the interaction between the SARS-CoV-2 Spike protein and the human ACE2 receptor is a promising therapeutic strategy. We designed inhibitors using two de novo design approaches. Computer generated scaffolds were either built around an ACE2 helix that interacts with the Spike receptor binding domain (RBD), or docked against the RBD to identify new binding modes, and their amino acid sequences designed to optimize target binding, folding and stability. Ten designs bound the RBD with affinities ranging from 100pM to 10nM, and blocked  ARS-CoV-2 infection of Vero E6 cells with IC 50 values between 24 pM and 35 nM; The most potent, with new binding modes, are 56 and 64 residue proteins (IC 50 ~ 0.16 ng/ml). Cryo-electron microscopy structures of these minibinders in complex with the SARS-CoV-2 spike ectodomain trimer with all three RBDs bound are nearly identical to the computational models. These hyperstable minibinders provide starting points for SARS-CoV-2 therapeutics.

DOI: 10.1126/science.abd9909

Source: https://science.sciencemag.org/content/early/2020/09/08/science.abd9909

期刊信息
Science:《科学》,创刊于1880年。隶属于美国科学促进会,最新IF:41.037