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埃可病毒和痘苗病毒干扰素-γ结合蛋白的种属特异性。

Species specificity of ectromelia virus and vaccinia virus interferon-gamma binding proteins.

作者信息

Mossman K, Upton C, Buller R M, McFadden G

机构信息

Department of Biochemistry, University of Alberta, Edmonton, Canada.

出版信息

Virology. 1995 Apr 20;208(2):762-9. doi: 10.1006/viro.1995.1208.

DOI:10.1006/viro.1995.1208
PMID:7747448
Abstract

Interferon-gamma functions within the immune system as a potent anti-viral and immunoregulatory cytokine. In order to successfully replicate within a host cell, poxviruses have evolved a number of strategies to counteract the pleiotropic effects of interferon-gamma. In particular, the leporipoxvirus myxoma virus was shown to express an extracellular soluble interferon-gamma receptor homolog, denoted M-T7, which is capable of inhibiting the anti-viral activities of rabbit interferon-gamma (C. Upton, K. Mossman, and G. McFadden, 1992, Science 258, 1369-1372). Here, we demonstrate that expression of soluble interferon-gamma receptor homologs appears to be characteristic of all poxviruses tested, including Shope fibroma virus, vaccinia virus (strains WR and IHDW), ectromelia virus, cowpox virus, and rabbitpox virus. We have cloned, sequenced, and characterized the interferon-gamma binding protein in supernatants from ectromelia virus-infected cells, and demonstrate the capability of this soluble protein to bind human, murine, and rabbit interferon-gamma with similar affinity. We also investigate the properties of the vaccinia virus interferon-gamma binding protein and demonstrate that this protein binds human and rabbit interferon-gamma with similar affinity and binds murine interferon-gamma with a significantly lower relative affinity. The implications of these studies with respect to viral pathogenesis and the evolutionary relationship between a virus and its host are discussed.

摘要

干扰素-γ在免疫系统中作为一种有效的抗病毒和免疫调节细胞因子发挥作用。为了在宿主细胞内成功复制,痘病毒已经进化出多种策略来对抗干扰素-γ的多效性作用。特别是,兔痘病毒黏液瘤病毒被证明表达一种细胞外可溶性干扰素-γ受体同源物,命名为M-T7,它能够抑制兔干扰素-γ的抗病毒活性(C.厄普顿、K.莫斯曼和G.麦克法登,1992年,《科学》258卷,1369 - 1372页)。在此,我们证明可溶性干扰素-γ受体同源物的表达似乎是所有测试痘病毒的特征,包括肖普纤维瘤病毒、痘苗病毒(WR株和IHDW株)、埃可病毒、牛痘病毒和兔痘病毒。我们已经克隆、测序并鉴定了来自埃可病毒感染细胞上清液中的干扰素-γ结合蛋白,并证明这种可溶性蛋白能够以相似的亲和力结合人、鼠和兔干扰素-γ。我们还研究了痘苗病毒干扰素-γ结合蛋白的特性,并证明该蛋白以相似的亲和力结合人和兔干扰素-γ,而以显著较低的相对亲和力结合鼠干扰素-γ。讨论了这些研究对病毒发病机制以及病毒与其宿主之间进化关系的影响。

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