Physico-Chemical Mechanisms of the Functioning of Membrane-Active Proteins of Enveloped Viruses

O. V. Batishchev
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Abstract

Over the past few years, the attention of the whole world has been riveted to the emergence of new dangerous strains of viruses, among which a special place is occupied by coronaviruses that have overcome the interspecies barrier in the past 20 years: SARS viruses (SARS), Middle East respiratory syndrome (MERS), as well as a new coronavirus infection (SARS-CoV-2), which caused the largest pandemic since the Spanish flu in 1918. Coronaviruses are members of a class of enveloped viruses that have a lipoprotein envelope. This class also includes such serious pathogens as human immunodeficiency virus (HIV), hepatitis, Ebola virus, influenza, etc. Despite significant differences in the clinical picture of the course of disease caused by enveloped viruses, they themselves have a number of characteristic features, which determine their commonality. Regardless of the way of penetration into the cell—by endocytosis or direct fusion with the cell membrane—enveloped viruses are characterized by the following stages of interaction with the target cell: binding to receptors on the cell surface, interaction of the surface glycoproteins of the virus with the membrane structures of the infected cell, fusion of the lipid envelope of the virion with plasma or endosomal membrane, destruction of the protein capsid and its dissociation from the viral nucleoprotein. Subsequently, within the infected cell, the newly synthesized viral proteins must self-assemble on various membrane structures to form a progeny virion. Thus, both the initial stages of viral infection and the assembly and release of new viral particles are associated with the activity of viral proteins in relation to the cell membrane and its organelles. This review is devoted to the analysis of physicochemical mechanisms of functioning of the main structural proteins of a number of enveloped viruses in order to identify possible strategies for the membrane activity of such proteins at various stages of viral infection of the cell.

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包膜病毒膜活性蛋白功能的理化机制
在过去的几年里,全世界的注意力都集中在新的危险病毒株的出现上,其中冠状病毒占据了一个特殊的位置,它们在过去的20年里克服了物种间的障碍:SARS病毒(SARS),中东呼吸综合征(MERS),以及一种新的冠状病毒感染(SARS- cov -2),它造成了自1918年西班牙流感以来最大规模的大流行。冠状病毒是一类具有脂蛋白包膜的病毒的成员。这一类还包括严重的病原体,如人类免疫缺陷病毒(HIV)、肝炎、埃博拉病毒、流感等。尽管包膜病毒引起的疾病过程的临床表现存在显著差异,但它们本身具有许多特征,这决定了它们的共性。无论渗透细胞的方式是内吞作用还是直接与细胞膜融合,包膜病毒与靶细胞的相互作用都有以下几个阶段:与细胞表面受体的结合,病毒表面糖蛋白与被感染细胞的膜结构的相互作用,病毒粒子的脂质包膜与血浆或内体膜的融合,蛋白质衣壳的破坏及其与病毒核蛋白的解离。随后,在被感染的细胞内,新合成的病毒蛋白必须在各种膜结构上自组装以形成子代病毒粒子。因此,病毒感染的初始阶段和新病毒颗粒的组装和释放都与与细胞膜及其细胞器相关的病毒蛋白的活性有关。本文对几种包膜病毒的主要结构蛋白的理化机制进行了分析,以确定这些蛋白在病毒感染细胞的不同阶段的膜活性的可能策略。
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来源期刊
CiteScore
1.40
自引率
0.00%
发文量
28
期刊介绍: Biochemistry (Moscow), Supplement Series A: Membrane and Cell Biology   is an international peer reviewed journal that publishes original articles on physical, chemical, and molecular mechanisms that underlie basic properties of biological membranes and mediate membrane-related cellular functions. The primary topics of the journal are membrane structure, mechanisms of membrane transport, bioenergetics and photobiology, intracellular signaling as well as membrane aspects of cell biology, immunology, and medicine. The journal is multidisciplinary and gives preference to those articles that employ a variety of experimental approaches, basically in biophysics but also in biochemistry, cytology, and molecular biology. The journal publishes articles that strive for unveiling membrane and cellular functions through innovative theoretical models and computer simulations.
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