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人类博卡病毒衣壳结构:对细小病毒科结构多样性的深入了解。

Human bocavirus capsid structure: insights into the structural repertoire of the parvoviridae.

机构信息

Department of Biochemistry and Molecular Biology, University of Florida, Gainesville, Florida 32610, USA.

出版信息

J Virol. 2010 Jun;84(12):5880-9. doi: 10.1128/JVI.02719-09. Epub 2010 Apr 7.

Abstract

Human bocavirus (HBoV) was recently discovered and classified in the Bocavirus genus (family Parvoviridae, subfamily Parvovirinae) on the basis of genomic similarity to bovine parvovirus and canine minute virus. HBoV has been implicated in respiratory tract infections and gastroenteric disease in children worldwide, yet despite numerous epidemiological reports, there has been limited biochemical and molecular characterization of the virus. Reported here is the three-dimensional structure of recombinant HBoV capsids, assembled from viral protein 2 (VP2), at 7.9-A resolution as determined by cryo-electron microscopy and image reconstruction. A pseudo-atomic model of HBoV VP2 was derived from sequence alignment analysis and knowledge of the crystal structure of human parvovirus B19 (genus Erythrovirus). Comparison of the HBoV capsid structure to that of parvoviruses from five separate genera demonstrates strong conservation of a beta-barrel core domain and an alpha-helix, from which emanate several loops of various lengths and conformations, yielding a unique surface topology that differs from the three already described for this family. The highly conserved core is consistent with observations for other single-stranded DNA viruses, and variable surface loops have been shown to confer the host-specific tropism and the diverse antigenic properties of this family.

摘要

人博卡病毒(HBoV)是最近在基于基因组与牛细小病毒和犬细小病毒相似性的基础上,在博卡病毒属(细小病毒科,细小病毒亚科)中被发现并分类的。HBoV 已被牵连到全球儿童的呼吸道感染和胃肠道疾病中,但尽管有许多流行病学报告,对该病毒的生化和分子特征的研究却很有限。这里报道的是通过冷冻电镜和图像重建,在 7.9-A 分辨率下确定的由病毒蛋白 2(VP2)组装的重组 HBoV 衣壳的三维结构。HBoV VP2 的拟原子模型是通过序列比对分析和对人细小病毒 B19(红病毒属)的晶体结构的了解推导出来的。将 HBoV 衣壳结构与来自五个不同属的细小病毒进行比较,显示出一个β桶核心域和一个α螺旋的强烈保守性,这些螺旋从其中伸出几个长度和构象不同的环,产生独特的表面拓扑结构,与该家族已经描述的三种结构不同。高度保守的核心与其他单链 DNA 病毒的观察结果一致,可变表面环已被证明赋予了宿主特异性嗜性和该家族的多样化抗原特性。

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