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口蹄疫病毒VP1 GH环对αv整合素的特异性

Specificity of the VP1 GH loop of Foot-and-Mouth Disease virus for alphav integrins.

作者信息

Burman Alison, Clark Stuart, Abrescia Nicola G A, Fry Elizabeth E, Stuart David I, Jackson Terry

机构信息

Division of Microbiology, Institute for Animal Health, Pirbright, Surrey, GU24 ONF, United Kingdom.

出版信息

J Virol. 2006 Oct;80(19):9798-810. doi: 10.1128/JVI.00577-06.

Abstract

Foot-and-mouth disease virus (FMDV) can use a number of integrins as receptors to initiate infection. Attachment to the integrin is mediated by a highly conserved arginine-glycine-aspartic acid (RGD) tripeptide located on the GH loop of VP1. Other residues of this loop are also conserved and may contribute to integrin binding. In this study we have used a 17-mer peptide, whose sequence corresponds to the GH loop of VP1 of type O FMDV, as a competitor of integrin-mediated virus binding and infection. Alanine substitution through this peptide identified the leucines at the first and fourth positions following RGD (RGD+1 and RGD+4 sites) as key for inhibition of virus binding and infection mediated by alphavbeta6 or alphavbeta8 but not for inhibition of virus binding to alphavbeta3. We also show that FMDV peptides containing either methionine or arginine at the RGD+1 site, which reflects the natural sequence variation seen across the FMDV serotypes, are effective inhibitors for alphavbeta6. In contrast, although RGDM-containing peptides were effective for alphavbeta8, RGDR-containing peptides were not. These observations were confirmed by showing that a virus containing an RGDR motif uses alphavbeta8 less efficiently than alphavbeta6 as a receptor for infection. Finally, evidence is presented that shows alphavbeta3 to be a poor receptor for infection by type O FMDV. Taken together, our data suggest that the integrin binding loop of FMDV has most likely evolved for binding to alphavbeta6 with a higher affinity than to alphavbeta3 and alphavbeta8.

摘要

口蹄疫病毒(FMDV)可利用多种整合素作为受体来启动感染。与整合素的结合由位于VP1的GH环上的高度保守的精氨酸 - 甘氨酸 - 天冬氨酸(RGD)三肽介导。该环的其他残基也保守,可能有助于整合素结合。在本研究中,我们使用了一种17肽,其序列对应于O型FMDV的VP1的GH环,作为整合素介导的病毒结合和感染的竞争者。通过该肽进行丙氨酸取代确定了RGD之后第一位和第四位的亮氨酸(RGD +1和RGD +4位点)是抑制由αvβ6或αvβ8介导的病毒结合和感染的关键,但不是抑制病毒与αvβ3结合的关键。我们还表明,在RGD +1位点含有甲硫氨酸或精氨酸的FMDV肽,反映了FMDV血清型中所见的天然序列变异,是αvβ6的有效抑制剂。相比之下,虽然含RGDM的肽对αvβ8有效,但含RGDR的肽则无效。通过显示含有RGDR基序的病毒比αvβ6更不有效地利用αvβ8作为感染受体,证实了这些观察结果。最后,有证据表明αvβ3是O型FMDV感染的不良受体。综上所述,我们的数据表明FMDV的整合素结合环最有可能进化为以比αvβ3和αvβ8更高的亲和力与αvβ6结合。

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