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Fas在人类胸腺细胞发育早期表达,但不传递凋亡信号。

Fas is expressed early in human thymocyte development but does not transmit an apoptotic signal.

作者信息

Jenkins M, Keir M, McCune J M

机构信息

Gladstone Institute of Virology and Immunology, Department of Medicine, University of California, San Francisco 94141, USA.

出版信息

J Immunol. 1999 Aug 1;163(3):1195-204.

Abstract

We investigated the expression and function of Fas on human thymocytes prepared from fetal and pediatric tissue specimens and from SCID-hu Thy/Liv grafts. Unlike mouse thymocytes, human thymocytes exhibited a pattern of Fas expression skewed to immature cells, in that the highest expression was seen on double negative thymocytes and on intrathymic T progenitor cells. Fas expression was intermediate on double positive human thymocytes, and low or negative on mature single positive CD4 and CD8 medullary thymocytes. In spite of this relatively abundant surface expression, cross-linking of Fas with agonist mAb was incapable of triggering an apoptotic signal in human thymocytes. Apoptotic signaling was not enhanced by treatment with cycloheximide, nor by restoring a cosignaling milieu by addition of thymic stromal cells. Mouse thymocytes were induced to apoptosis by cross-linked recombinant soluble human Fas ligand both in vitro and in vivo, though human thymocytes were also resistant to this mode of receptor ligation. Membrane-bound Fas ligand also induced apoptotic death in murine thymocytes but not in human thymocytes. Human thymocytes were as sensitive as Jurkat cells, however, to apoptosis induced by TNF-alpha, suggesting that these cells have a signaling defect before activation of the earliest caspases. These data demonstrate a durable and specific resistance of human thymocytes to apoptosis induced through Fas receptor engagement, and reveal significant species-specific differences in the biology of thymocyte-programmed cell death.

摘要

我们研究了Fas在从胎儿和儿科组织标本以及严重联合免疫缺陷-人胸腺/肝脏移植物制备的人胸腺细胞中的表达和功能。与小鼠胸腺细胞不同,人胸腺细胞呈现出Fas表达偏向未成熟细胞的模式,即双阴性胸腺细胞和胸腺内T祖细胞上的表达最高。Fas在双阳性人胸腺细胞上的表达处于中等水平,而在成熟的单阳性CD4和CD8髓质胸腺细胞上表达低或为阴性。尽管表面表达相对丰富,但用激动剂单克隆抗体交联Fas无法在人胸腺细胞中触发凋亡信号。用环己酰亚胺处理或通过添加胸腺基质细胞恢复共信号环境均不能增强凋亡信号。体外和体内实验中,交联的重组可溶性人Fas配体可诱导小鼠胸腺细胞凋亡,不过人胸腺细胞对这种受体连接方式也具有抗性。膜结合Fas配体也可诱导小鼠胸腺细胞凋亡,但不能诱导人胸腺细胞凋亡。然而,人胸腺细胞与Jurkat细胞一样,对TNF-α诱导的凋亡敏感,这表明这些细胞在最早的半胱天冬酶激活之前存在信号缺陷。这些数据证明了人胸腺细胞对通过Fas受体结合诱导的凋亡具有持久而特异性的抗性,并揭示了胸腺细胞程序性细胞死亡生物学中显著的物种特异性差异。

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