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马疱疹病毒 4 型利用一组有限的马主要组织相容性复合体 I 类蛋白作为进入受体。

Equid herpesvirus type 4 uses a restricted set of equine major histocompatibility complex class I proteins as entry receptors.

机构信息

Department of Virology, Faculty of Veterinary Medicine, Zagazig University, Zagazig, Egypt.

Institut für Virologie, Robert von Ostertag-Haus, Zentrum für Infektionsmedizin, Freie Universität Berlin, 14163 Berlin, Germany.

出版信息

J Gen Virol. 2014 Jul;95(Pt 7):1554-1563. doi: 10.1099/vir.0.066407-0. Epub 2014 Apr 10.

Abstract

Equid herpesvirus type 1 (EHV-1) was shown to use an unusual receptor for cellular entry - MHC-I molecules. Here, we demonstrated that the closely related EHV, EHV-4, also uses this strategy for cellular invasion, both in equine cells in culture and in the heterologous, non-permissive murine mastocytoma cell line (P815) after stable transfection with horse MHC-I genes. Using a panel of P815 cell lines transfected with individual horse MHC-I genes, we provided support for the hypothesis that EHV-1 and EHV-4 target classical polymorphic MHC-I molecules as viral entry receptors. All known equine MHC-I molecules from the two principal classical polymorphic loci specify alanine at position 173 (A173), whilst other MHC-I loci encoded different amino acids at this position and did not permit viral entry. Site-directed mutagenesis of position 173 diminished or enhanced viral entry, depending upon the initial amino acid. However, there were other, as yet undefined, constraints to this process: MHC-I genes from two non-classical loci carried A173 but did not enable viral entry in P815 transfectants. Our study suggested that the capacity to bind MHC-I molecules arose in the common ancestor of EHV-1 and EHV-4. The widespread occurrence of A173 in classical polymorphic horse MHC-I molecules indicated that horses of most MHC haplotypes should be susceptible to infection via this entry portal.

摘要

马疱疹病毒 1 型(EHV-1)已被证明使用一种不寻常的细胞进入受体——MHC-I 分子。在这里,我们证明了密切相关的 EHV-4 也使用这种策略进行细胞入侵,无论是在培养的马细胞中,还是在稳定转染马 MHC-I 基因的异源、非允许的鼠肥大细胞瘤系(P815)中。使用一组转染了单个马 MHC-I 基因的 P815 细胞系,我们为 EHV-1 和 EHV-4 以经典多态性 MHC-I 分子作为病毒进入受体的假说提供了支持。两个主要的经典多态性位点的所有已知马 MHC-I 分子在位置 173 指定丙氨酸(A173),而其他 MHC-I 位点在此位置编码不同的氨基酸,不允许病毒进入。位置 173 的定点突变减少或增强了病毒进入,这取决于初始氨基酸。然而,这个过程还有其他尚未定义的限制:来自两个非经典位点的 MHC-I 基因携带 A173,但不能使 P815 转染子中的病毒进入。我们的研究表明,结合 MHC-I 分子的能力出现在 EHV-1 和 EHV-4 的共同祖先中。A173 在经典多态性马 MHC-I 分子中的广泛存在表明,大多数 MHC 单倍型的马都应该容易通过这种进入门户感染。

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