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参与人类T淋巴细胞激活的细胞表面分子和早期事件。

Cell surface molecules and early events involved in human T lymphocyte activation.

作者信息

Weiss A, Imboden J B

机构信息

Department of Medicine, Howard Hughes Medical Institute, University of California, San Francisco 94143.

出版信息

Adv Immunol. 1987;41:1-38. doi: 10.1016/s0065-2776(08)60029-2.

Abstract

The physiologic activation of human T cells by antigen involves events that occur between ligands and receptors at the interface of the T cell and antigen-presenting cell (or target cell). These events have been examined by identifying the cell surface receptors involved in such interactions using mAb. Whereas the T3/T cell antigen receptor plays a central role in such interactions, other T cell receptors have been identified which may also contribute to T cell activation in providing primary activation signals or by functioning as accessory molecules. Although the ligands of these other receptors are currently unknown or ill defined, it is likely that this will provide a fruitful area of investigation. The use of mAb as probes to mimic these putative ligands has facilitated the study of the requirements for activation and the biochemical events initiated by the receptors involved. The T cell receptor, a multisubunit complex, has been most intensively studied. Ligands that bind to T3/Ti cannot initiate activation by themselves and require the participation of accessory molecules. Stimulation of T3/Ti results in the formation of at least two potent intracellular second messengers, IP3 and DG, through the hydrolysis of PIP2. These second messengers, in turn, induce an increase in [Ca2+]i and the activation of pkC. These two events appear to be essential in the transcriptional activation of certain targeted genes through ill-defined pathways leading to the manifestations of T cell activation.

摘要

抗原对人T细胞的生理性激活涉及T细胞与抗原呈递细胞(或靶细胞)界面处配体与受体之间发生的事件。通过使用单克隆抗体鉴定参与此类相互作用的细胞表面受体,对这些事件进行了研究。虽然T3/T细胞抗原受体在此类相互作用中起核心作用,但已鉴定出其他T细胞受体,它们也可能在提供初始激活信号或作为辅助分子发挥作用时,对T细胞激活有贡献。尽管这些其他受体的配体目前尚不清楚或定义不明确,但这可能会成为一个富有成果的研究领域。使用单克隆抗体作为探针来模拟这些假定的配体,有助于研究激活的要求以及相关受体引发的生化事件。T细胞受体是一种多亚基复合物,已得到最深入的研究。与T3/Ti结合的配体自身不能引发激活,需要辅助分子的参与。T3/Ti的刺激通过PIP2的水解导致至少两种有效的细胞内第二信使IP3和DG的形成。这些第二信使进而诱导细胞内钙离子浓度升高和蛋白激酶C的激活。这两个事件似乎对于通过不明确的途径导致T细胞激活表现的某些靶向基因的转录激活至关重要。

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