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利用可选择的山羊关节炎-脑炎病毒假型系统确定小反刍兽慢病毒细胞病变变体的宿主范围。

Host range of small-ruminant lentivirus cytopathic variants determined with a selectable caprine arthritis- encephalitis virus pseudotype system.

作者信息

Hötzel I, Cheevers W P

机构信息

Department of Veterinary Microbiology and Pathology, Washington State University, Pullman, Washington 99164-7040, USA.

出版信息

J Virol. 2001 Aug;75(16):7384-91. doi: 10.1128/JVI.75.16.7384-7391.2001.

Abstract

The small-ruminant lentiviruses ovine maedi-visna virus (MVV) and caprine arthritis-encephalitis virus (CAEV) cause encephalitis, progressive pneumonia, arthritis, and mastitis in sheep and goats. Icelandic MVV strains, which are lytic in tissue culture, have a wide species distribution of functional receptors, which includes human cells. In contrast, functional receptors for the nonlytic CAEV CO are absent from human cells. To determine if the wide species distribution of functional receptors is a common property of MVV strains or related to cytopathic phenotype, we tested the infectivity of viruses pseudotyped with the envelope glycoproteins of MVV K1514, CAEV CO, and lytic and nonlytic North American MVV strains to cells of different species. Replication-defective CAEV proviral constructs lacking the env, tat, and vif genes and carrying the neomycin phosphotransferase gene in the vif-tat region were developed for the infectivity assays. Cotransfection of human 293T cells with these proviral constructs and plasmids expressing CAEV, MVV, or vesicular stomatitis virus envelope glycoproteins produced infectious pseudotyped virus which induced resistance of infected cells to G418. Using these pseudotypes, we confirmed the wide species distribution of Icelandic MVV receptors and the narrow host range of CAEV. However, functional receptors for the two North American MVV strains tested, unlike the Icelandic MVV and similar to CAEV, were limited to cells of ruminant species, regardless of cytopathic phenotype. The results indicate a differential receptor recognition by MVV strains which is unrelated to cytopathic phenotype.

摘要

小反刍兽慢病毒绵羊梅迪 - 维斯纳病毒(MVV)和山羊关节炎 - 脑炎病毒(CAEV)可在绵羊和山羊中引发脑炎、进行性肺炎、关节炎和乳腺炎。冰岛的MVV毒株在组织培养中具有溶解性,其功能性受体具有广泛的物种分布,包括人类细胞。相比之下,人类细胞中不存在非溶解性CAEV CO的功能性受体。为了确定功能性受体的广泛物种分布是MVV毒株的共同特性还是与细胞病变表型相关,我们测试了用MVV K1514、CAEV CO以及溶解性和非溶解性北美MVV毒株的包膜糖蛋白假型化的病毒对不同物种细胞的感染性。为进行感染性测定,构建了缺失env、tat和vif基因且在vif - tat区域携带新霉素磷酸转移酶基因的复制缺陷型CAEV前病毒构建体。将这些前病毒构建体与表达CAEV、MVV或水疱性口炎病毒包膜糖蛋白的质粒共转染人293T细胞,产生了感染性假型病毒,该病毒可诱导感染细胞对G418产生抗性。利用这些假型,我们证实了冰岛MVV受体的广泛物种分布以及CAEV的狭窄宿主范围。然而,与冰岛MVV不同且与CAEV类似,所测试的两种北美MVV毒株的功能性受体仅限于反刍动物物种的细胞,无论其细胞病变表型如何。结果表明MVV毒株存在不同的受体识别方式,这与细胞病变表型无关。

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