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单纯疱疹病毒特异性人类细胞毒性T细胞中CD4+CD8-和CD8+CD4-的体外差异激活

Differential in vitro activation of CD4+CD8- and CD8+CD4- herpes simplex virus-specific human cytotoxic T cells.

作者信息

Yasukawa M, Inatsuki A, Kobayashi Y

机构信息

First Department of Internal Medicine, Ehime University School of Medicine, Japan.

出版信息

J Immunol. 1989 Sep 15;143(6):2051-7.

PMID:2476493
Abstract

In order to clarify the differential activation of CD4+ and CD8+ HSV-specific CTL, we compared the characteristics of CTL generated by different methods of in vitro HSV stimulation by treatment of effectors with anti-CD4 and anti-CD8 mAb and C after the elimination of nonspecific cytotoxic effector cells. Cell-free HSV mainly activated CD4+ CTL precursors, whereas HSV-infected fibroblasts were more effective in activating CD8+ CTL precursors than CD4+ CTL precursors. In addition, limiting dilution analyses with enriched T cells from two HSV-seropositive donors revealed that the frequency of HSV-specific CD4+ CTL precursors responsive to stimulation with free HSV was approximately 1/4,000 to 6,000 CD4+ T cells, whereas that of precursors responsive to stimulation with HSV-infected fibroblasts was approximately 1/19,000 to 22,000 CD4+ T cells. Conversely, the frequency of CD8+ CTL precursors in peripheral blood responsive to stimulation with free HSV was approximately 1/28,000 to 30,000 CD8+ T cells, whereas that of precursors responsive to stimulation with HSV-infected fibroblasts was approximately 1/10,000 to 11,000 CD8+ T cells. The present data suggest that generalized viral infection due to cell-free viruses is fought mainly by CD4+ CTL, which have previously been reported to possess both cytotoxicity and helper function, and that localized viral infection on HLA class II-negative fibroblasts is prevented from spreading to adjacent cells mainly by CD8+ CTL. Such differential activation of CD4+ and CD8+ CTL seems probable when considering the protective mechanisms against viral infection.

摘要

为了阐明CD4⁺和CD8⁺单纯疱疹病毒(HSV)特异性细胞毒性T淋巴细胞(CTL)的差异激活情况,我们在用抗CD4和抗CD8单克隆抗体及补体(C)处理效应细胞以消除非特异性细胞毒性效应细胞后,比较了不同体外HSV刺激方法所产生的CTL的特征。无细胞HSV主要激活CD4⁺CTL前体,而HSV感染的成纤维细胞在激活CD8⁺CTL前体方面比激活CD4⁺CTL前体更有效。此外,对来自两名HSV血清阳性供体的富集T细胞进行有限稀释分析发现,对无细胞HSV刺激有反应的HSV特异性CD4⁺CTL前体频率约为每4000至6000个CD4⁺T细胞中有1个,而对HSV感染的成纤维细胞刺激有反应的前体频率约为每19000至22000个CD4⁺T细胞中有1个。相反,外周血中对无细胞HSV刺激有反应的CD8⁺CTL前体频率约为每28000至30000个CD8⁺T细胞中有1个,而对HSV感染的成纤维细胞刺激有反应的前体频率约为每10000至11000个CD8⁺T细胞中有1个。目前的数据表明,无细胞病毒引起的全身性病毒感染主要由CD4⁺CTL对抗,此前报道CD4⁺CTL兼具细胞毒性和辅助功能,而HLA II类阴性成纤维细胞上的局部病毒感染主要通过CD8⁺CTL防止扩散到相邻细胞。考虑到针对病毒感染的保护机制,CD4⁺和CD8⁺CTL的这种差异激活似乎是合理的。

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