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一种γ疱疹病毒分泌的Vβ4 + CD8 + T细胞激活剂可调节慢性感染和免疫病理学。

A gammaherpesvirus-secreted activator of Vbeta4+ CD8+ T cells regulates chronic infection and immunopathology.

作者信息

Evans Andrew G, Moser Janice M, Krug Laurie T, Pozharskaya Veranika, Mora Ana L, Speck Samuel H

机构信息

Emory Vaccine Center, Department of Microbiology and Immunology, Emory University School of Medicine, Atlanta, GA 30322, USA.

出版信息

J Exp Med. 2008 Mar 17;205(3):669-84. doi: 10.1084/jem.20071135. Epub 2008 Mar 10.

DOI:10.1084/jem.20071135
PMID:18332178
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2275388/
Abstract

Little is known about herpesvirus modulation of T cell activation in latently infected individuals or the implications of such for chronic immune disorders. Murine gammaherpesvirus 68 (MHV68) elicits persistent activation of CD8(+) T cells bearing a Vbeta4(+) T cell receptor (TCR) by a completely unknown mechanism. We show that a novel MHV68 protein encoded by the M1 gene is responsible for Vbeta4(+) CD8(+) T cell stimulation in a manner reminiscent of a viral superantigen. During infection, M1 expression induces a Vbeta4(+) effector T cell response that resists functional exhaustion and appears to suppress virus reactivation from peritoneal cells by means of long-term interferon-gamma (IFNgamma) production. Mice lacking an IFNgamma receptor (IFNgammaR(-/-)) fail to control MHV68 replication, and Vbeta4(+) and CD8(+) T cell activation by M1 instead contributes to severe inflammation and multiorgan fibrotic disease. Thus, M1 manipulates the host CD8(+) T cell response in a manner that facilitates latent infection in an immunocompetent setting, but promotes disease during a dysregulated immune response. Identification of a viral pathogenecity determinant with superantigen-like activity for CD8(+) T cells broadens the known repertoire of viral immunomodulatory molecules, and its function illustrates the delicate balance achieved between persistent viruses and the host immune response.

摘要

对于潜伏感染个体中疱疹病毒对T细胞激活的调节作用,以及这对慢性免疫紊乱的影响,我们知之甚少。小鼠γ疱疹病毒68(MHV68)通过一种完全未知的机制引发携带Vβ4(+) T细胞受体(TCR)的CD8(+) T细胞的持续激活。我们发现,由M1基因编码的一种新型MHV68蛋白以类似于病毒超抗原的方式负责刺激Vβ4(+) CD8(+) T细胞。在感染过程中,M1的表达诱导Vβ4(+)效应T细胞反应,该反应可抵抗功能耗竭,并似乎通过长期产生干扰素-γ(IFNγ)来抑制腹膜细胞中的病毒再激活。缺乏IFNγ受体的小鼠(IFNγR(-/-))无法控制MHV68的复制,而M1对Vβ4(+)和CD8(+) T细胞的激活反而导致严重炎症和多器官纤维化疾病。因此,M1以一种促进免疫健全环境中潜伏感染,但在免疫反应失调期间促进疾病发展的方式操纵宿主CD8(+) T细胞反应。鉴定出一种对CD8(+) T细胞具有超抗原样活性的病毒致病性决定因素,拓宽了已知的病毒免疫调节分子库,其功能说明了持续性病毒与宿主免疫反应之间实现的微妙平衡。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4120/2275388/e434a1ba8279/jem2050669f08.jpg
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