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“CD3低表达”的人类胸腺细胞群体可通过CD2和/或CD28激活途径轻易被触发,而CD3途径仍无功能。

"CD3low" human thymocyte populations can readily be triggered via the CD2 and/or CD28 activation pathways whereas the CD3 pathway remains nonfunctional.

作者信息

Pierres A, Cerdan C, Lopez M, Mawas C, Olive D

机构信息

Unité de Cancérologie et Thérapeutique Experimentale, U. 119 Inserm, Marseille, France.

出版信息

J Immunol. 1990 Feb 15;144(4):1202-7.

PMID:1968076
Abstract

We have investigated the role of the CD2 and the CD28 Ag-independent pathways of activation on CD3low thymocytes. We previously showed that anti-CD28 mAb synergized with anti-CD2 mAb directed against epitopes T11.1 and T11.2, in the activation of purified resting T cells or unseparated thymocytes. Proliferation induced via CD2 plus CD28 was mediated via an IL-2-dependent pathway and was not affected by prior modulation of the CD3-TCR complex. Here, we show that a subset of CD3low thymocytes, although unresponsive to CD3 activation, can be activated to proliferate through the CD2 or the CD28 pathways, in the presence of exogenous IL-2. The mitogenic combination of mAb to CD2 and CD28 induces a proliferation of thymocytes which, in absence of exogenous lymphokines, is restricted to the more mature intrathymic subpopulation, CD1a-. However, CD3low thymocytes can also be triggered through the CD2 plus CD28 activation pathways but require at least addition of exogenous IL-2 to proliferate. This study demonstrates that a fraction of immature CD3low thymocytes possesses functional CD2 and CD28 surface molecules at a time when CD3 is not yet functional.

摘要

我们研究了CD2和CD28非抗原依赖性激活途径在CD3低表达胸腺细胞中的作用。我们先前表明,抗CD28单克隆抗体与针对表位T11.1和T11.2的抗CD2单克隆抗体协同作用,激活纯化的静息T细胞或未分离的胸腺细胞。通过CD2加CD28诱导的增殖是通过IL-2依赖性途径介导的,并且不受CD3-TCR复合物先前调节的影响。在此,我们表明,尽管对CD3激活无反应,但CD3低表达胸腺细胞的一个亚群在存在外源性IL-2的情况下可通过CD2或CD28途径被激活而增殖。抗CD2和CD28单克隆抗体的促有丝分裂组合诱导胸腺细胞增殖,在没有外源性淋巴因子的情况下,这种增殖仅限于胸腺内更成熟的亚群CD1a-。然而,CD3低表达胸腺细胞也可通过CD2加CD28激活途径被触发,但需要至少添加外源性IL-2才能增殖。这项研究表明,一部分未成熟的CD3低表达胸腺细胞在CD3尚未发挥功能时就具有功能性的CD2和CD28表面分子。

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