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衣壳化货物的长度影响体外组装的甲病毒核心样颗粒的稳定性和结构。

Length of encapsidated cargo impacts stability and structure of in vitro assembled alphavirus core-like particles.

作者信息

Rayaprolu Vamseedhar, Moore Alan, Wang Joseph Che-Yen, Goh Boon Chong, Perilla Juan R, Zlotnick Adam, Mukhopadhyay Suchetana

机构信息

Departments of Biology, Indiana University, Bloomington, IN, United States of America.

出版信息

J Phys Condens Matter. 2017 Dec 6;29(48):484003. doi: 10.1088/1361-648X/aa90d0.

Abstract

In vitro assembly of alphavirus nucleocapsid cores, called core-like particles (CLPs), requires a polyanionic cargo. There are no sequence or structure requirements to encapsidate single-stranded nucleic acid cargo. In this work, we wanted to determine how the length of the cargo impacts the stability and structure of the assembled CLPs. We hypothesized that cargo neutralizes the basic region of the alphavirus capsid protein and if the cargo is long enough, it will also act to scaffold the CP monomers together. Experimentally we found that CLPs encapsidating short 27mer oligonucleotides were less stable than CLPs encapsidating 48mer or 90mer oligonucleotides under different chemical and thermal conditions. Furthermore, cryo-EM studies showed there were structural differences between CLPs assembled with 27mer and 48mer cargo. To mimic the role of the cargo in CLP assembly we made a mutant (4D) where we substituted a cluster of four Lys residues in the CP with four Asp residues. We found that these few amino acid substitutions were enough to initiate CLP assembly in the absence of cargo. The cargo-free 4D CLPs show higher resistance to ionic strength and increased temperature compared to wild-type cargo containing CLPs suggesting their CLP assembly mechanism might also be different.

摘要

甲病毒核衣壳核心(称为类核心颗粒,CLPs)的体外组装需要一种聚阴离子货物。对于包裹单链核酸货物,不存在序列或结构要求。在这项工作中,我们想确定货物的长度如何影响组装好的CLPs的稳定性和结构。我们假设货物中和了甲病毒衣壳蛋白的碱性区域,并且如果货物足够长,它还将起到将衣壳蛋白单体聚集在一起的支架作用。通过实验我们发现,在不同的化学和热条件下,包裹短27聚体寡核苷酸的CLPs比包裹48聚体或90聚体寡核苷酸的CLPs更不稳定。此外,冷冻电镜研究表明,由27聚体和48聚体货物组装而成的CLPs之间存在结构差异。为了模拟货物在CLP组装中的作用,我们构建了一个突变体(4D),其中我们将衣壳蛋白中的四个赖氨酸残基簇替换为四个天冬氨酸残基。我们发现,这几个氨基酸取代足以在没有货物的情况下启动CLP组装。与含有野生型货物的CLPs相比,无货物的4D CLPs对离子强度和温度升高表现出更高的抗性,这表明它们的CLP组装机制可能也不同。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8025/7103146/c826622cde04/cmaa90d0f01_pr.jpg

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