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抗玻连蛋白受体(整合素αVβ3)的抗体可抑制口蹄疫病毒与培养细胞的结合及感染。

Antibodies to the vitronectin receptor (integrin alpha V beta 3) inhibit binding and infection of foot-and-mouth disease virus to cultured cells.

作者信息

Berinstein A, Roivainen M, Hovi T, Mason P W, Baxt B

机构信息

Plum Island Animal Disease Center, Agricultural Research Service, U.S. Department of Agriculture, Greenport, New York 11944.

出版信息

J Virol. 1995 Apr;69(4):2664-6. doi: 10.1128/JVI.69.4.2664-2666.1995.

Abstract

The amino acid sequence Arg-Gly-Asp (RGD) is highly conserved on the VP1 proteins of different serotypes and subtypes of foot-and-mouth disease virus (FMDV) and is essential for cell attachment. This sequence is also found in certain extracellular matrix proteins that bind to a family of cell surface receptors called integrins. Within the Picornaviridae family, enterovirus coxsackievirus A9 also has an RGD motif on its VP1 capsid protein and has recently been shown to utilize the vitronectin receptor integrin alpha V beta 3 as a receptor on monkey kidney cells. Competition binding experiments between type A12 FMDV and coxsackievirus A9 using BHK-21 and LLC-MK2 cells revealed shared receptor specificity between these two viruses. Polyclonal anti-serum to the vitronectin receptor and a monoclonal antibody to the alpha V subunit inhibited both FMDV binding and plaque formation, while a monoclonal antibody to the beta 3 subunit inhibited virus binding. In contrast, antibodies to the fibronectin receptor (alpha 5 beta 1) or to the integrin (alpha V beta 5) had no effect on either binding or plaque formation. These data demonstrate that the alpha V beta 3 vitronectin receptor can function as a receptor for FMDV.

摘要

精氨酸-甘氨酸-天冬氨酸(RGD)氨基酸序列在口蹄疫病毒(FMDV)不同血清型和亚型的VP1蛋白上高度保守,且对细胞黏附至关重要。该序列也存在于某些与一类称为整合素的细胞表面受体结合的细胞外基质蛋白中。在小RNA病毒科中,肠道病毒柯萨奇病毒A9在其VP1衣壳蛋白上也有一个RGD基序,最近已证明它在猴肾细胞上利用玻连蛋白受体整合素αVβ3作为受体。使用BHK-21和LLC-MK2细胞对A12型FMDV和柯萨奇病毒A9进行的竞争结合实验揭示了这两种病毒之间存在共同的受体特异性。针对玻连蛋白受体的多克隆抗血清和针对αV亚基的单克隆抗体抑制了FMDV的结合和蚀斑形成,而针对β3亚基的单克隆抗体抑制了病毒结合。相比之下,针对纤连蛋白受体(α5β1)或整合素(αVβ5)的抗体对结合或蚀斑形成均无影响。这些数据表明,αVβ3玻连蛋白受体可作为FMDV的受体发挥作用。

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