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白细胞介素2的低亲和力和高亲和力细胞受体。对Tac抗原水平的影响。

Low and high affinity cellular receptors for interleukin 2. Implications for the level of Tac antigen.

作者信息

Robb R J, Greene W C, Rusk C M

出版信息

J Exp Med. 1984 Oct 1;160(4):1126-46. doi: 10.1084/jem.160.4.1126.

Abstract

Interleukin 2 promotes proliferation of T cells by virtue of its interaction with a high-affinity cell surface receptor. This receptor is a 55,000 mol wt glycoprotein that is also recognized by the murine monoclonal antibody, anti-Tac. Quantitative binding studies with radiolabeled IL-2 and anti-Tac, however, initially indicated far more antibody binding sites per cell than IL-2 binding sites. Extension of the IL-2 binding analysis to concentrations several thousand-fold higher than that necessary for the T cell proliferative response demonstrated the existence of a class (or classes) of low-affinity IL-2 binding sites. Inclusion of the low-affinity IL-2 binding greatly reduced the quantitative discrepancy in the ligand binding assays. That the low-affinity binding, as well as the high-affinity interaction, was associated with the Tac molecule was indicated by the finding that the antibody could substantially or totally block the entire spectrum of IL-2 binding and by the finding that IL-2 could in turn block all radiolabeled anti-Tac binding. The low-affinity sites were found on activated T cells, several human and murine T cell lines and two examples of Tac-positive B cells. The physiological role of the low-affinity IL-2 binding sites and the molecular changes in the Tac protein that give rise to the affinity differences remain open to investigation.

摘要

白细胞介素2通过与高亲和力细胞表面受体相互作用促进T细胞增殖。该受体是一种分子量为55,000的糖蛋白,也可被鼠单克隆抗体抗-Tac识别。然而,用放射性标记的白细胞介素2和抗-Tac进行的定量结合研究最初表明,每个细胞的抗体结合位点比白细胞介素2结合位点多得多。将白细胞介素2结合分析扩展到比T细胞增殖反应所需浓度高数千倍的浓度,证明存在一类低亲和力的白细胞介素2结合位点。低亲和力白细胞介素2结合的存在大大减少了配体结合试验中的定量差异。抗体可基本上或完全阻断白细胞介素2结合的整个范围,以及白细胞介素2可反过来阻断所有放射性标记的抗-Tac结合,这一发现表明低亲和力结合以及高亲和力相互作用都与Tac分子有关。在活化的T细胞、几种人和鼠T细胞系以及两个Tac阳性B细胞实例中发现了低亲和力位点。低亲和力白细胞介素2结合位点的生理作用以及导致亲和力差异的Tac蛋白的分子变化仍有待研究。

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