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人鼻病毒 C 衣壳的建模提示了一种新的拓扑结构,为受体偏好性和免疫原性提供了新的见解。

Modeling of the human rhinovirus C capsid suggests a novel topography with insights on receptor preference and immunogenicity.

机构信息

Institute for Molecular Virology, University of Wisconsin, Madison, USA.

出版信息

Virology. 2014 Jan 5;448:176-84. doi: 10.1016/j.virol.2013.10.006. Epub 2013 Oct 25.

Abstract

Features of human rhinovirus (RV)-C virions that allow them to use novel cell receptors and evade immune responses are unknown. Unlike the RV-A+B, these isolates cannot be propagated in typical culture systems or grown for structure studies. Comparative sequencing, I-TASSER, MODELLER, ROBETTA, and refined alignment techniques led to a structural approximation for C15 virions, based on the extensive, resolved RV-A+B datasets. The model predicts that all RV-C VP1 proteins are shorter by 21 residues relative to the RV-A, and 35 residues relative to the RV-B, effectively shaving the RV 5-fold plateau from the particle. There are major alterations in VP1 neutralizing epitopes and the structural determinants for ICAM-1 and LDLR receptors. The VP2 and VP3 elements are similar among all RV, but the loss of sequence "words" contributing Nim1ab has increased the apparent selective pressure among the RV-C to fix mutations elsewhere in the VP1, creating a possible compensatory epitope.

摘要

人类鼻病毒(RV)-C 病毒粒子的特征使得它们能够使用新型细胞受体并逃避免疫反应,这一点尚不清楚。与 RV-A+B 不同,这些分离株不能在典型的培养系统中繁殖,也不能用于结构研究。比较测序、I-TASSER、MODELLER、ROBETTA 和改进的对齐技术,基于广泛的、已解决的 RV-A+B 数据集,为 C15 病毒粒子提供了结构近似。该模型预测,所有的 RV-C VP1 蛋白相对于 RV-A 短 21 个残基,相对于 RV-B 短 35 个残基,有效地将 RV 的 5 倍平台从粒子上削去。VP1 中和表位和 ICAM-1 和 LDLR 受体的结构决定因素发生了重大改变。所有 RV 中的 VP2 和 VP3 元素都相似,但序列“单词”的缺失导致 Nim1ab 的缺失增加了 RV-C 中其他地方固定突变的选择压力,创造了一个可能的补偿表位。

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