定量蛋白质组学分析原发性 T 细胞信号osome 动力学,鉴定表面受体 CD6 作为 Lat 衔接子非依赖性 TCR 信号枢纽。
Quantitative proteomics analysis of signalosome dynamics in primary T cells identifies the surface receptor CD6 as a Lat adaptor-independent TCR signaling hub.
机构信息
Centre d'Immunologie de Marseille-Luminy, UM2 Aix-Marseille Université, Marseille, France.
INSERM U1104, Marseille, France.
出版信息
Nat Immunol. 2014 Apr;15(4):384-392. doi: 10.1038/ni.2843. Epub 2014 Mar 2.
Abstract
T cell antigen receptor (TCR)-mediated activation of T cells requires the interaction of dozens of proteins. Here we used quantitative mass spectrometry and activated primary CD4(+) T cells from mice in which a tag for affinity purification was knocked into several genes to determine the composition and dynamics of multiprotein complexes that formed around the kinase Zap70 and the adaptors Lat and SLP-76. Most of the 112 high-confidence time-resolved protein interactions we observed were previously unknown. The surface receptor CD6 was able to initiate its own signaling pathway by recruiting SLP-76 and the guanine nucleotide-exchange factor Vav1 regardless of the presence of Lat. Our findings provide a more complete model of TCR signaling in which CD6 constitutes a signaling hub that contributes to the diversification of TCR signaling.
摘要
T 细胞抗原受体 (TCR) 介导的 T 细胞激活需要数十种蛋白质的相互作用。在这里,我们使用定量质谱法和经过激活的来自敲入多个基因标签的小鼠的原代 CD4(+) T 细胞,来确定围绕激酶 Zap70 和衔接蛋白 Lat 和 SLP-76 形成的多蛋白复合物的组成和动态。我们观察到的 112 个高可信度的时程分辨蛋白相互作用中,大多数以前都不知道。表面受体 CD6 能够通过招募 SLP-76 和鸟嘌呤核苷酸交换因子 Vav1 来启动其自身的信号通路,而不管 Lat 的存在与否。我们的研究结果提供了一个更完整的 TCR 信号模型,其中 CD6 构成了一个信号枢纽,有助于 TCR 信号的多样化。
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