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鼠诺如病毒 NS1-2 蛋白的固有结构无序和二聚化。

Inherent structural disorder and dimerisation of murine norovirus NS1-2 protein.

机构信息

Department of Microbiology and Immunology, University of Otago, Dunedin, New Zealand.

出版信息

PLoS One. 2012;7(2):e30534. doi: 10.1371/journal.pone.0030534. Epub 2012 Feb 7.

DOI:10.1371/journal.pone.0030534
PMID:22347381
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3274520/
Abstract

Human noroviruses are highly infectious viruses that cause the majority of acute, non-bacterial epidemic gastroenteritis cases worldwide. The first open reading frame of the norovirus RNA genome encodes for a polyprotein that is cleaved by the viral protease into six non-structural proteins. The first non-structural protein, NS1-2, lacks any significant sequence similarity to other viral or cellular proteins and limited information is available about the function and biophysical characteristics of this protein. Bioinformatic analyses identified an inherently disordered region (residues 1-142) in the highly divergent N-terminal region of the norovirus NS1-2 protein. Expression and purification of the NS1-2 protein of Murine norovirus confirmed these predictions by identifying several features typical of an inherently disordered protein. These were a biased amino acid composition with enrichment in the disorder promoting residues serine and proline, a lack of predicted secondary structure, a hydrophilic nature, an aberrant electrophoretic migration, an increased Stokes radius similar to that predicted for a protein from the pre-molten globule family, a high sensitivity to thermolysin proteolysis and a circular dichroism spectrum typical of an inherently disordered protein. The purification of the NS1-2 protein also identified the presence of an NS1-2 dimer in Escherichia coli and transfected HEK293T cells. Inherent disorder provides significant advantages including structural flexibility and the ability to bind to numerous targets allowing a single protein to have multiple functions. These advantages combined with the potential functional advantages of multimerisation suggest a multi-functional role for the NS1-2 protein.

摘要

人类诺如病毒是高度传染性的病毒,可导致全球大多数急性非细菌性流行胃肠炎病例。诺如病毒 RNA 基因组的第一个开放阅读框编码一个多蛋白,该多蛋白被病毒蛋白酶切割成六个非结构蛋白。第一个非结构蛋白 NS1-2 与其他病毒或细胞蛋白没有明显的序列相似性,关于该蛋白的功能和生物物理特性的信息有限。生物信息学分析鉴定出诺如病毒 NS1-2 蛋白高度变异的 N 端区域存在一个固有无序区域(残基 1-142)。鼠诺如病毒 NS1-2 蛋白的表达和纯化通过鉴定几个固有无序蛋白的典型特征证实了这些预测。这些特征包括具有丰富的无序促进残基丝氨酸和脯氨酸的偏性氨基酸组成、缺乏预测的二级结构、亲水性、异常的电泳迁移、增加的斯托克斯半径类似于前熔融球蛋白家族的蛋白质的预测值、对胰凝乳蛋白酶的高敏感性以及固有无序蛋白的典型圆二色性光谱。NS1-2 蛋白的纯化还鉴定出在大肠杆菌和转染的 HEK293T 细胞中存在 NS1-2 二聚体。固有无序提供了显著的优势,包括结构灵活性和结合众多靶标的能力,使单个蛋白质具有多种功能。这些优势与多聚化的潜在功能优势相结合,表明 NS1-2 蛋白具有多功能作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c2e9/3274520/7f7c201d4bbf/pone.0030534.g008.jpg
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