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首页> 外文期刊>The Journal of Experomental Medicine >The Transmembrane Adaptor Protein Trim Regulates T Cell Receptor (Tcr) Expression and Tcr-Mediated Signaling via an Association with the Tcr ζ Chain
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The Transmembrane Adaptor Protein Trim Regulates T Cell Receptor (Tcr) Expression and Tcr-Mediated Signaling via an Association with the Tcr ζ Chain

机译:跨膜衔接蛋白修饰通过与Tcrζ链缔合来调节T细胞受体(Tcr)表达和Tcr介导的信号传导。

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摘要

T cell receptor (TCR)-interacting molecule (TRIM) is a recently identified transmembrane adaptor protein, which is exclusively expressed in T cells. Here we demonstrate that in mature T cells, TRIM preferentially interacts with the TCR via the TCR - ζ chains and to a lesser extent via the CD3-ε/γ heterodimer. Transient or stable overexpression of TRIM in Jurkat T cells results in enhancement of TCR expression on the cell surface and elevated induction of Ca2+ mobilization after T cell activation. TRIM-mediated upregulation of TCR expression results from inhibition of spontaneous TCR internalization and stabilization of TCR complexes on the cell surface. Collectively, our data identify TRIM as a novel integral component of the TCR complex and suggest that one function of TRIM might be to modulate the strength of signals transduced through the TCR through regulation of TCR expression on the cell surface.
机译:T细胞受体(TCR)相互作用分子(TRIM)是最近鉴定的跨膜衔接蛋白,仅在T细胞中表达。在这里,我们证明,在成熟的T细胞中,TRIM优先通过TCR-ζ链与TCR相互作用,并在较小程度上通过CD3-ε/γ异二聚体与TCR相互作用。 TRIM激活后,Jurkat T细胞中TRIM的瞬时或稳定过表达导致TCR在细胞表面的表达增强和Ca2 +动员的诱导增强。 TRIM介导的TCR表达上调是由于抑制了自发的TCR内在化和细胞表面TCR复合物的稳定。总的来说,我们的数据将TRIM识别为TCR复合体的新型组成部分,并暗示TRIM的功能之一可能是通过调节细胞表面TCR的表达来调节通过TCR传导的信号强度。

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