设计和测试干扰 SARS-CoV-2 穗状病毒蛋白与其宿主细胞受体之间识别机制的分子

IF 5.6 2区 化学 Q1 CHEMISTRY, MEDICINAL Journal of Chemical Information and Modeling Pub Date : 2024-10-23 DOI:10.1021/acs.jcim.4c01511
Francesca Scantamburlo, Ionica Masgras, Francesco Ciscato, Claudio Laquatra, Francesco Frigerio, Fabrizio Cinquini, Silvia Pavoni, Alice Triveri, Elena Frasnetti, Stefano A. Serapian, Giorgio Colombo, Andrea Rasola, Elisabetta Moroni
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摘要

COVID-19 大流行所造成的破坏性影响促使科学界做出了前所未有的努力,以确定病毒感染机制的特征。其中,病毒糖基化穗状病毒与人类受体 ACE2 和 TMPRSS2 之间的相互作用是病毒入侵的关键。在这里,我们报告并测试了一种完全合理的方法,用于设计能够扰乱 SARS-CoV-2 致病性中这些关键角色之间相互作用的分子。为此,我们通过计算确定了全糖基化 Spike 蛋白上未进行分子内优化的亚结构,这些亚结构容易通过与 ACE2 和 TMPRSS2 形成复合物而被稳定。为了与 Spike 介导的细胞进入机制竞争,我们以肽模拟物的形式设计了预测的假定相互作用区域,这些肽模拟物可以与 Spike 竞争与 ACE2 和/或 TMPRSS2 的相互作用。病毒进入细胞的实验模型表明,所设计的分子能够干扰病毒进入表达 ACE2/TMPRSS2 的细胞,而对不携带 Spike 蛋白的对照病毒颗粒的进入或 Spike 呈递的病毒颗粒进入表面不显示其受体的细胞则没有影响。
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Design and Test of Molecules that Interfere with the Recognition Mechanisms between the SARS-CoV-2 Spike Protein and Its Host Cell Receptors
The disruptive impact of the COVID-19 pandemic has led the scientific community to undertake an unprecedented effort to characterize viral infection mechanisms. Among these, interactions between the viral glycosylated Spike and the human receptors ACE2 and TMPRSS2 are key to allowing virus invasion. Here, we report and test a fully rational methodology to design molecules that are capable of perturbing the interactions between these critical players in SARS-CoV-2 pathogenicity. To this end, we computationally identify substructures on the fully glycosylated Spike protein that are not intramolecularly optimized and are thus prone to being stabilized by forming complexes with ACE2 and TMPRSS2. With the aim of competing with the Spike-mediated cell entry mechanisms, we have engineered the predicted putative interaction regions in the form of peptide mimics that could compete with Spike for interaction with ACE2 and/or TMPRSS2. Experimental models of viral entry demonstrate that the designed molecules are able to interfere with viral entry into ACE2/TMPRSS2 expressing cells, while they have no effects on the entry of control viral particles that do not harbor the Spike protein or on the entry of Spike-presenting viral particles into cells that do not display its receptors on their surface.
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来源期刊
CiteScore
9.80
自引率
10.70%
发文量
529
审稿时长
1.4 months
期刊介绍: The Journal of Chemical Information and Modeling publishes papers reporting new methodology and/or important applications in the fields of chemical informatics and molecular modeling. Specific topics include the representation and computer-based searching of chemical databases, molecular modeling, computer-aided molecular design of new materials, catalysts, or ligands, development of new computational methods or efficient algorithms for chemical software, and biopharmaceutical chemistry including analyses of biological activity and other issues related to drug discovery. Astute chemists, computer scientists, and information specialists look to this monthly’s insightful research studies, programming innovations, and software reviews to keep current with advances in this integral, multidisciplinary field. As a subscriber you’ll stay abreast of database search systems, use of graph theory in chemical problems, substructure search systems, pattern recognition and clustering, analysis of chemical and physical data, molecular modeling, graphics and natural language interfaces, bibliometric and citation analysis, and synthesis design and reactions databases.
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