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首页> 外文期刊>Journal of Virology >CD8-positive T lymphocytes specific for murine cytomegalovirus immediate-early antigens mediate protective immunity.
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CD8-positive T lymphocytes specific for murine cytomegalovirus immediate-early antigens mediate protective immunity.

机译:CD8阳性T淋巴细胞特异于鼠塞细胞病毒立即早期抗原调解保护免疫。

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We have shown in a murine model system for acute, lethal cytomegalovirus (CMV) disease in the immunocompromised natural host that control of virus multiplication in tissues, protection from virus-caused tissue destruction, and survival are mediated by virus-specific CD8+ CD4-T lymphocytes. Protection from a lethal course of disease did not result in a rapid establishment of virus latency, but led to a long-lasting, persistent state of infection. The CD8- CD4+ subset of T lymphocytes was not effective by itself in controlling murine CMV (MCMV) multiplication in tissue or essential for the protective function of the CD8+ CD4- effector cells. The antiviral efficacy of the purified CD8+ CD4- subset was not impaired by preincubation with fibroblasts that presented viral structural antigens, but was significantly reduced after depletion of effector cells specific for the nonstructural immediate-early antigens of MCMV, which are specified by the first among a multitude of viral genes expressed during MCMV replication in permissive cells. Thus, MCMV disease provides the first example of a role for nonstructural herpesvirus immediate-early antigens in protective immunity.
机译:我们在免疫致致致死的患有免疫致致死的胞嘧啶病毒(CMV)疾病中的鼠模型系统中显示了控制病毒繁殖在组织中,保护免受病毒导致的组织破坏,并通过病毒特异性CD8 + CD4-T介导的存活率淋巴细胞。从致命的疾病方案的保护并没有导致病毒潜伏期的快速建立,但导致了持久的持续感染状态。 T淋巴细胞的CD8- CD4 +副本本身无效地控制组织中的鼠CMV(MCMV)倍增,或者对于CD8 + CD4-效应细胞的保护功能必不可少。纯化的CD8 + CD4-子集的抗病毒功效不是通过对呈递病毒结构抗原的成纤维细胞预孵育的抗病毒功效,但在MCMV的非结构立即早期抗原特异的效应细胞耗尽后显着降低,这是由第一个指定的在允许细胞中的MCMV复制期间表达了多种病毒基因。因此,MCMV疾病提供了非结构疱疹病毒立即抗原在保护性免疫中的作用的第一个例子。

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