Single-domain antibody for binding the conserved epitope in the SARS-CoV-2 spike protein receptor-binding domain

IF 0.2 Q4 MEDICINE, GENERAL & INTERNAL Bulletin of Russian State Medical University Pub Date : 2023-02-01 DOI:10.24075/brsmu.2023.005
P. Vorobyev, SV Tillib
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Abstract

Several COVID-19 vaccines have been developed in the last three years using various tecnhiques. Multiple virus-neutralizing antibodies against SARS-CoV-2 have been also obtained to combat the pandemic. However, the use of these medications for prevention and potential treatment faces significant challenges due to the emergence of new mutant virus variants, both more contagious and escaping neutralization by the immune system, that is why it is necessary to continuously renew the vaccines and develop new therapeutic antibodies. The study was aimed to use the technology of generating single-domain antibodies (nanobodies) to target the surface spike (S) protein RBD conserved epitope of the broad spectrum of SARS-CoV-2 variants. Recombinant proteins that corresponded to RBDs of three important SARS-СoV-2 strains and the full-length S protein (Wuhan) were used as antigens for immunization of a camel in order to induce production of appropriate antibodies and/or as immobilized proteins for further cross selection of the nanobody clones with pre-set specificity by the phage display. A nanobody capable of effectively recognizing the conservative region in the S protein RBDs of the broad spectrum of pandemic SARS-CoV-2 variants, including Omicron, was selected from the generated immune library. Along with conventional use in immunoassays and diagnosis, the generated nanobody can be potentially used as a module for target-specific binding used to trap coronavirus in human upper airways during the development of novel combination antiviral drugs.
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结合SARS-CoV-2刺突蛋白受体结合域保守表位的单域抗体
在过去三年中,使用各种技术开发了几种COVID-19疫苗。针对SARS-CoV-2的多种病毒中和抗体也已获得,以对抗大流行。然而,由于新的突变病毒变体的出现,这些药物用于预防和潜在治疗面临着重大挑战,这些突变病毒变体更具传染性,并且逃避免疫系统的中和,这就是为什么有必要不断更新疫苗并开发新的治疗性抗体。本研究旨在利用产生单域抗体(纳米体)的技术,靶向SARS-CoV-2广谱变异的表面刺突(S)蛋白RBD保守表位。利用三种重要SARS-СoV-2毒株RBDs对应的重组蛋白和全长S蛋白(武汉)作为骆驼免疫抗原,诱导产生合适的抗体和/或作为固定蛋白,通过噬菌体展示对具有预先设定特异性的纳米体克隆进行进一步交叉选择。从生成的免疫文库中选择了一个能够有效识别包括Omicron在内的大流行SARS-CoV-2变体的广谱S蛋白rbd中的保守区域的纳米体。除了在免疫分析和诊断中的常规用途外,所生成的纳米体还可能在开发新型联合抗病毒药物期间用作靶向特异性结合的模块,用于在人类上呼吸道中捕获冠状病毒。
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来源期刊
Bulletin of Russian State Medical University
Bulletin of Russian State Medical University MEDICINE, GENERAL & INTERNAL-
CiteScore
0.80
自引率
0.00%
发文量
59
期刊介绍: Bulletin of Russian State Medical University (Bulletin of RSMU, ISSN Print 2500–1094, ISSN Online 2542–1204) is a peer-reviewed medical journal of Pirogov Russian National Research Medical University (Moscow, Russia). The original language of the journal is Russian (Vestnik Rossiyskogo Gosudarstvennogo Meditsinskogo Universiteta, Vestnik RGMU, ISSN Print 2070–7320, ISSN Online 2070–7339). Founded in 1994, it is issued once every two months publishing articles on clinical medicine and medical and biological sciences, first of all oncology, neurobiology, allergy and immunology, medical genetics, medical microbiology and infectious diseases. Every issue is thematic. Deadlines for manuscript submission are announced in advance. The number of publications on topics in spite of the issue topic is limited. The journal accepts only original articles submitted by their authors, including articles that present methods and techniques, clinical cases and opinions. Authors must guarantee that their work has not been previously published elsewhere in whole or in part and in other languages and is not under consideration by another scientific journal. The journal publishes only one review per issue; the review is ordered by the editors.
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