在体内经历超抗原诱导凋亡的外周T细胞表达B220并上调Fas和Fas配体。
Peripheral T cells undergoing superantigen-induced apoptosis in vivo express B220 and upregulate Fas and Fas ligand.
作者信息
Renno T, Hahne M, Tschopp J, MacDonald H R
机构信息
Ludwig Institute for Cancer Research, University of Lausanne, Epalinges, Switzerland.
出版信息
J Exp Med. 1996 Feb 1;183(2):431-7. doi: 10.1084/jem.183.2.431.
Abstract
Staphylococcal enterotoxin B (SEB) is a bacterial superantigen (SAg) that predominantly interacts with V(beta)8+ T cells. In vivo treatment of mice with SEB leads to an initial increase in the percentage of V(beta)8+ T cells, followed by a decrease in the numbers of these cells, eventually reaching lower levels than those found before treatment with the SAg. This decrease is due to apoptosis of the SEB-responding cells. In the present study, we use the distinct light scattering characteristics of apoptotic cells to characterize T cells that are being deleted in response to SEB in vivo. We show that dying, SEB-reactive T cells express high levels of Fas and Fas ligand (Fas-L), which are implicated in apoptotic cell death. In addition, the B cell marker B220 is upregulated on apoptotic cells. Moreover, we show that the generation of cells with an apoptotic phenotype is severely impaired in response to SEB in functional Fas-L-deficient mutant gld mice, confirming the role of the Fas pathway in SAg mediated peripheral deletion in vivo.
摘要
葡萄球菌肠毒素B(SEB)是一种主要与Vβ8 + T细胞相互作用的细菌超抗原(SAg)。用SEB对小鼠进行体内治疗会导致Vβ8 + T细胞百分比最初增加,随后这些细胞数量减少,最终降至低于用该SAg治疗前的水平。这种减少是由于对SEB有反应的细胞发生凋亡。在本研究中,我们利用凋亡细胞独特的光散射特性来表征体内因SEB而被清除的T细胞。我们发现,濒死的、对SEB有反应的T细胞表达高水平的Fas和Fas配体(Fas-L),这与凋亡性细胞死亡有关。此外,B细胞标志物B220在凋亡细胞上上调。而且,我们发现,在功能性Fas-L缺陷的突变型gld小鼠中,对SEB有反应的具有凋亡表型的细胞生成严重受损,这证实了Fas途径在体内SAg介导的外周细胞清除中的作用。
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