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T细胞抗原受体化学计量学:为提高敏感性进行预聚集

T-cell antigen-receptor stoichiometry: pre-clustering for sensitivity.

作者信息

Alarcón Balbino, Swamy Mahima, van Santen Hisse M, Schamel Wolfgang W A

机构信息

Centro de Biología Molecular Severo Ochoa, CSIC-Universidad Autónoma de Madrid, Madrid 28049, Spain.

出版信息

EMBO Rep. 2006 May;7(5):490-5. doi: 10.1038/sj.embor.7400682.

Abstract

The T-cell antigen receptor (TCR x CD3) is a multi-subunit complex that is responsible for triggering an adaptive immune response. It shows high specificity and sensitivity, while having a low affinity for the ligand. Furthermore, T cells respond to antigen over a wide concentration range. The stoichiometry and architecture of TCR x CD3 in the membrane have been under intense scrutiny because they might be the key to explaining its paradoxical properties. This review highlights new evidence that TCR x CD3 is found on intact unstimulated T cells in a monovalent form (one ligand-binding site per receptor) as well as in several distinct multivalent forms. This is in contrast to the TCR x CD3 stoichiometries determined by several biochemical means; however, these data can be explained by the effects of different detergents on the integrity of the receptor. Here, we discuss a model in which the multivalent receptors are important for the detection of low concentrations of ligand and therefore confer sensitivity, whereas the co-expressed monovalent TCR x CD3s allow a wide dynamic range.

摘要

T细胞抗原受体(TCR×CD3)是一种多亚基复合体,负责触发适应性免疫反应。它具有高特异性和敏感性,但对配体的亲和力较低。此外,T细胞能在很宽的浓度范围内对抗原作出反应。膜中TCR×CD3的化学计量和结构一直受到密切关注,因为它们可能是解释其矛盾特性的关键。本综述强调了新的证据,即TCR×CD3以单价形式(每个受体一个配体结合位点)以及几种不同的多价形式存在于完整的未刺激T细胞上。这与通过几种生化方法确定的TCR×CD3化学计量相反;然而,这些数据可以通过不同去污剂对受体完整性的影响来解释。在此,我们讨论一种模型,其中多价受体对于低浓度配体的检测很重要,因此赋予了敏感性,而共表达的单价TCR×CD3则允许较宽的动态范围。

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