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噬菌体φX174的DNA包装中间体

DNA packaging intermediates of bacteriophage φX174.

作者信息

Ilag Leodevico L, Olson Norman H, Dokland Terje, Music Cynthia L, Cheng R Holland, Bowen Zorina, McKenna Robert, Rossmann Michael G, Baker Timothy S, Incardona Nino L

机构信息

Department of Biological Sciences, Purdue University, West Lafayette, IN 47907-1392, USA.

Department of Microbiology and Immunology, Center for the Health Sciences, University of Tennessee, 858 Madison Avenue, Memphis, TN 38163, USA.

出版信息

Structure. 1995 Apr 15;3(4):353-363. doi: 10.1016/S0969-2126(01)00167-8.

Abstract

BACKGROUND

Like many viruses, bacteriophage phi X174 packages its DNA genome into a procapsid that is assembled from structural intermediates and scaffolding proteins. The procapsid contains the structural proteins F, G and H, as well as the scaffolding proteins B and D. Provirions are formed by packaging of DNA together with the small internal J proteins, while losing at least some of the B scaffolding proteins. Eventually, loss of the D scaffolding proteins and the remaining B proteins leads to the formation of mature virions.

RESULTS

phi X174 108S 'procapsids' have been purified in milligram quantities by removing 114S (mature virion) and 70S (abortive capsid) particles from crude lysates by differential precipitation with polyethylene glycol. 132S 'provirions' were purified on sucrose gradients in the presence of EDTA. Cryo-electron microscopy (cryo-EM) was used to obtain reconstructions of procapsids and provirions. Although these are very similar to each other, their structures differ greatly from that of the virion. The F and G proteins, whose atomic structures in virions were previously determined from X-ray crystallography, were fitted into the cryo-EM reconstructions. This showed that the pentamer of G proteins on each five-fold vertex changes its conformation only slightly during DNA packaging and maturation, whereas major tertiary and quaternary structural changes occur in the F protein. The procapsids and provirions were found to contain 120 copies of the D protein arranged as tetramers on the two-fold axes. DNA might enter procapsids through one of the 30 A diameter holes on the icosahedral three-fold axes.

CONCLUSIONS

Combining cryo-EM image reconstruction and X-ray crystallography has revealed the major conformational changes that can occur in viral assembly. The function of the scaffolding proteins may be, in part, to support weak interactions between the structural proteins in the procapsids and to cover surfaces that are subsequently required for subunit-subunit interaction in the virion. The structures presented here are, therefore, analogous to chaperone proteins complexed with folding intermediates of a substrate.

摘要

背景

与许多病毒一样,噬菌体φX174将其DNA基因组包装到一个由结构中间体和支架蛋白组装而成的原衣壳中。原衣壳包含结构蛋白F、G和H,以及支架蛋白B和D。前病毒体是通过将DNA与小的内部J蛋白一起包装形成的,同时至少损失一些B支架蛋白。最终,D支架蛋白和剩余的B蛋白的损失导致成熟病毒体的形成。

结果

通过用聚乙二醇进行差异沉淀,从粗裂解物中去除114S(成熟病毒体)和70S(流产衣壳)颗粒,以毫克量纯化了φX174 108S“原衣壳”。在EDTA存在下,通过蔗糖梯度纯化132S“前病毒体”。使用冷冻电子显微镜(cryo-EM)获得原衣壳和前病毒体的重建结构。尽管它们彼此非常相似,但它们的结构与病毒体的结构有很大不同。先前通过X射线晶体学确定了病毒体中原子结构的F和G蛋白,被拟合到冷冻电子显微镜重建结构中。这表明每个五重顶点上的G蛋白五聚体在DNA包装和成熟过程中仅略微改变其构象,而F蛋白则发生主要的三级和四级结构变化。发现原衣壳和前病毒体在二重轴上包含120个以四聚体形式排列的D蛋白拷贝。DNA可能通过二十面体三重轴上直径为30 Å的孔之一进入原衣壳。

结论

结合冷冻电子显微镜图像重建和X射线晶体学揭示了病毒组装过程中可能发生的主要构象变化。支架蛋白的功能可能部分是支持原衣壳中结构蛋白之间的弱相互作用,并覆盖病毒体中亚基-亚基相互作用随后所需的表面。因此,这里呈现的结构类似于与底物折叠中间体复合的伴侣蛋白。

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