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腺相关病毒衣壳结构与细胞相互作用。

AAV capsid structure and cell interactions.

作者信息

Agbandje-McKenna Mavis, Kleinschmidt Jürgen

机构信息

Department of Biochemistry and Molecular Biology, University of Florida, Gainesville, FL, USA.

出版信息

Methods Mol Biol. 2011;807:47-92. doi: 10.1007/978-1-61779-370-7_3.

Abstract

The Adeno-associated viruses (AAVs) are not associated with any diseases, and their ability to package non-genomic DNA and to transduce different cell/tissue populations has generated significant interest in understanding their basic biology in efforts to improve their utilization for corrective gene delivery. This includes their capsid structure, cellular tropism and interactions for entry, uncoating, replication, DNA packaging, capsid assembly, and antibody neutralization. The human and nonhuman primate AAVs are clustered into serologically distinct genetic clade and serotype groups, which have distinct cellular/tissue tropisms and transduction efficiencies. These properties are highly dependent upon the AAV capsid amino acid sequence, their capsid structure, and their interactions with host cell factors, including cell surface receptors, co-receptors, signaling molecules, proteins involved in host DNA replication, and host-derived antibodies. This chapter reviews the current structural information on AAV capsids and the capsid viral protein regions playing a role in the cellular interactions conferring an infective phenotype, which are then used to annotate the functional regions of the capsid. Based on the current data, the indication is that the AAVs, like other members of the Parvoviridae and other ssDNA viruses that form a T = 1 capsid, have evolved a multifunctional capsid with conserved core regions as is required for efficient capsid trafficking, capsid assembly, and genome packaging. Disparate surface loop structures confer differential receptor recognition and are involved in antibody recognition. The role of structural regions in capsid uncoating remains to be elucidated.

摘要

腺相关病毒(AAV)与任何疾病均无关联,其包装非基因组DNA以及转导不同细胞/组织群体的能力,引发了人们对了解其基本生物学特性的浓厚兴趣,以便努力改进其在矫正基因递送中的应用。这包括它们的衣壳结构、细胞嗜性以及进入、脱壳、复制、DNA包装、衣壳组装和抗体中和等过程中的相互作用。人类和非人类灵长类动物的AAV被聚类为血清学上不同的遗传进化枝和血清型组,它们具有不同的细胞/组织嗜性和转导效率。这些特性高度依赖于AAV衣壳氨基酸序列、其衣壳结构以及它们与宿主细胞因子的相互作用,包括细胞表面受体、共受体、信号分子、参与宿主DNA复制的蛋白质以及宿主来源的抗体。本章综述了关于AAV衣壳的当前结构信息以及在赋予感染表型的细胞相互作用中起作用的衣壳病毒蛋白区域,然后用这些信息注释衣壳的功能区域。根据目前的数据,迹象表明,AAV与细小病毒科的其他成员以及形成T = 1衣壳的其他单链DNA病毒一样,已经进化出一种具有保守核心区域的多功能衣壳,这是衣壳有效运输、衣壳组装和基因组包装所必需的。不同的表面环结构赋予不同的受体识别能力,并参与抗体识别。衣壳结构区域在脱壳中的作用仍有待阐明。

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