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在内质网中组装的T细胞受体-CD3复合物及关键中间体的化学计量学。

Stoichiometry of the T-cell receptor-CD3 complex and key intermediates assembled in the endoplasmic reticulum.

作者信息

Call Matthew E, Pyrdol Jason, Wucherpfennig Kai W

机构信息

Department of Cancer Immunology & AIDS, Dana-Farber Cancer Institute, Boston, MA 02115, USA.

出版信息

EMBO J. 2004 Jun 16;23(12):2348-57. doi: 10.1038/sj.emboj.7600245. Epub 2004 May 20.

Abstract

The T-cell receptor (TCR)-CD3 complex is critical for T-cell development and function, and represents one of the most complex transmembrane receptors. Models of different stoichiometry and valency have been proposed based on cellular experiments and these have important implications for the mechanisms of receptor triggering. Since determination of receptor stoichiometry in T-cells is not possible due to the presence of previously synthesized, unlabeled receptor components with different half-lives, we examined the stoichiometry of the receptor assembled in endoplasmic reticulum (ER) microsomes of B-cell origin. The stoichiometric relationship among all subunits was directly determined using intact radiolabeled TCR-CD3 complexes that were isolated with a sequential, non-denaturing immunoprecipitation method, and identical results were obtained with two detergents belonging to different structural classes. The results firmly establish that the alphabeta TCR-CD3 complex assembled in the ER is monovalent and composed of one copy of the TCRalphabeta, CD3deltaepsilon, CD3gammaepsilon and zeta-zeta dimers.

摘要

T细胞受体(TCR)-CD3复合物对T细胞的发育和功能至关重要,是最复杂的跨膜受体之一。基于细胞实验提出了不同化学计量和价态的模型,这些模型对受体触发机制具有重要意义。由于存在先前合成的、具有不同半衰期的未标记受体成分,无法确定T细胞中受体的化学计量,因此我们研究了在B细胞来源的内质网(ER)微粒体中组装的受体的化学计量。使用完整的放射性标记TCR-CD3复合物,通过连续的非变性免疫沉淀方法进行分离,直接确定了所有亚基之间的化学计量关系,并且使用属于不同结构类别的两种去污剂获得了相同的结果。结果明确证实,在内质网中组装的αβ TCR-CD3复合物是单价的,由一份TCRαβ、CD3δε、CD3γε和ζ-ζ二聚体组成。

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