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腺病毒结构与装配的最新研究进展。

Latest insights on adenovirus structure and assembly.

机构信息

Department of Macromolecular Structures, Centro Nacional de Biotecnología (CNB-CSIC), Darwin 3, 28049 Madrid, Spain.

出版信息

Viruses. 2012 May;4(5):847-77. doi: 10.3390/v4050847. Epub 2012 May 21.

Abstract

Adenovirus (AdV) capsid organization is considerably complex, not only because of its large size (~950 Å) and triangulation number (pseudo T = 25), but also because it contains four types of minor proteins in specialized locations modulating the quasi-equivalent icosahedral interactions. Up until 2009, only its major components (hexon, penton, and fiber) had separately been described in atomic detail. Their relationships within the virion, and the location of minor coat proteins, were inferred from combining the known crystal structures with increasingly more detailed cryo-electron microscopy (cryoEM) maps. There was no structural information on assembly intermediates. Later on that year, two reports described the structural differences between the mature and immature adenoviral particle, starting to shed light on the different stages of viral assembly, and giving further insights into the roles of core and minor coat proteins during morphogenesis [1,2]. Finally, in 2010, two papers describing the atomic resolution structure of the complete virion appeared [3,4]. These reports represent a veritable tour de force for two structural biology techniques: X-ray crystallography and cryoEM, as this is the largest macromolecular complex solved at high resolution by either of them. In particular, the cryoEM analysis provided an unprecedented clear picture of the complex protein networks shaping the icosahedral shell. Here I review these latest developments in the field of AdV structural studies.

摘要

腺病毒(AdV)衣壳结构非常复杂,不仅因为其体积较大(~950Å)且正二十面体的三角数(pseudo T = 25)较高,还因为其在特定位置含有四种类型的调节准等价二十面体相互作用的次要蛋白。直到 2009 年,只有其主要成分(六邻体、五邻体和纤维)才分别以原子细节的形式被描述过。它们在病毒粒子中的关系,以及次要衣壳蛋白的位置,是通过将已知的晶体结构与越来越详细的冷冻电子显微镜(cryoEM)图谱结合起来推断的。对于组装中间体,没有结构信息。同年晚些时候,有两项报告描述了成熟和不成熟腺病毒颗粒之间的结构差异,开始揭示病毒组装的不同阶段,并进一步深入了解核心和次要衣壳蛋白在形态发生过程中的作用[1,2]。最后,在 2010 年,有两篇描述完整病毒粒子的原子分辨率结构的论文出现[3,4]。这些报告代表了两种结构生物学技术的真正杰作:X 射线晶体学和 cryoEM,因为这是它们中任何一种方法以高分辨率解决的最大的大分子复合物。特别是,cryoEM 分析提供了一个前所未有的清晰的复杂蛋白质网络,这些网络塑造了二十面体壳。在此,我回顾了 AdV 结构研究领域的这些最新进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e43f/3386624/1b5914b95e27/viruses-04-00847-g001.jpg

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