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在腺病毒6埃分辨率的冷冻电子显微镜结构中对α-螺旋的可视化,有助于优化衣壳蛋白的分配。

Visualization of alpha-helices in a 6-angstrom resolution cryoelectron microscopy structure of adenovirus allows refinement of capsid protein assignments.

作者信息

Saban Susan D, Silvestry Mariena, Nemerow Glen R, Stewart Phoebe L

机构信息

Vanderbilt University Medical Center, Department of Molecular Physiology and Biophysics, 710 Light Hall, 2215 Garland Ave., Nashville, TN 37232, USA.

出版信息

J Virol. 2006 Dec;80(24):12049-59. doi: 10.1128/JVI.01652-06. Epub 2006 Sep 27.

DOI:10.1128/JVI.01652-06
PMID:17005667
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1676273/
Abstract

The structure of adenovirus was determined to a resolution of 6 A by cryoelectron microscopy (cryoEM) single-particle image reconstruction. Docking of the hexon and penton base crystal structures into the cryoEM density established that alpha-helices of 10 or more residues are resolved as rods. A difference map was calculated by subtracting a pseudoatomic capsid from the cryoEM reconstruction. The resulting density was analyzed in terms of observed alpha-helices and secondary structure predictions for the additional capsid proteins that currently lack atomic resolution structures (proteins IIIa, VI, VIII, and IX). Protein IIIa, which is predicted to be highly alpha-helical, is assigned to a cluster of helices observed below the penton base on the inner capsid surface. Protein VI is present in approximately 1.5 copies per hexon trimer and is predicted to have two long alpha-helices, one of which appears to lie inside the hexon cavity. Protein VIII is cleaved by the adenovirus protease into two fragments of 7.6 and 12.1 kDa, and the larger fragment is predicted to have one long alpha-helix, in agreement with the observed density for protein VIII on the inner capsid surface. Protein IX is predicted to have one long alpha-helix, which also has a strongly indicated propensity for coiled-coil formation. A region of density near the facet edge is now resolved as a four-helix bundle and is assigned to four copies of the C-terminal alpha-helix from protein IX.

摘要

通过冷冻电子显微镜(cryoEM)单颗粒图像重建技术,腺病毒的结构被解析到了6埃的分辨率。将六邻体和五邻体基座晶体结构对接至cryoEM密度图中,确定10个或更多残基的α螺旋被解析为棒状结构。通过从cryoEM重建图像中减去一个伪原子衣壳来计算差异图。根据观察到的α螺旋以及目前缺乏原子分辨率结构的其他衣壳蛋白(蛋白IIIa、VI、VIII和IX)的二级结构预测,对所得密度进行分析。预测高度α螺旋化的蛋白IIIa被定位在内衣壳表面五邻体基座下方观察到的一组螺旋中。每个六邻体三聚体中大约有1.5个蛋白VI拷贝,预测其有两个长α螺旋,其中一个似乎位于六邻体腔内。腺病毒蛋白酶将蛋白VIII切割成7.6 kDa和12.1 kDa的两个片段,预测较大片段有一个长α螺旋,这与在内衣壳表面观察到的蛋白VIII密度一致。预测蛋白IX有一个长α螺旋,其也强烈倾向于形成卷曲螺旋。现在小面边缘附近的一个密度区域被解析为一个四螺旋束,并被指定为来自蛋白IX的C末端α螺旋的四个拷贝。

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The coiled-coil domain of the adenovirus type 5 protein IX is dispensable for capsid incorporation and thermostability.5型腺病毒蛋白IX的卷曲螺旋结构域对于衣壳掺入和热稳定性而言并非必需。
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