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首页> 外文期刊>Journal of proteome research >Vav1 Regulates T-Cell Activation through a Feedback Mechanism and Crosstalk between the T-Cell Receptor and CD28
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Vav1 Regulates T-Cell Activation through a Feedback Mechanism and Crosstalk between the T-Cell Receptor and CD28

机译:Vav1通过反馈机制和T细胞受体与CD28之间的串扰来调节T细胞活化

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Vav1, a Rac/Rho guanine nucleotide exchange factor and a critical component of the T-cell receptor (TCR) signaling cascade is tyrosine phosphorylated rapidly in response to T-cell activation. Vav1 has established roles in proliferation, cytokine secretion, Ca2+ responses, and actin cytoskeleton regulation; however, its function in the regulation of phosphorylation of TCR components, including the zeta chain, the CD3 delta, epsilon, gamma chains, and the associated kinases Lck and ZAP-70, is not well established. To obtain a more comprehensive picture of the role of Vavl in receptor proximal sighaling, we performed a wide-scale characterization of Vavl-dependent tyrosine phosphorylation events using quantitative phosphoproteomic analysis of VavI-deficient T cells across a time course of TCR stimulation. Importantly, this study revealed a new function for Vav1 in the negative feedback regulation of the phosphorylation of immunoreceptor tyrosine-based activation motifs within the chains, CD3 delta, epsilon, gamma chains, as well as activation sites on the critical T cell tyrosine kinases Itk, Lck, and ZAP-70. Our study also uncovered a previously unappreciated role for Vavl in crosstalk between the CD28 and TCR signaling pathways.
机译:Vav1,Rac / Rho鸟嘌呤核苷酸交换因子和T细胞受体(TCR)信号级联的关键组成部分响应T细胞活化而被酪氨酸快速磷酸化。 Vav1在增殖,细胞因子分泌,Ca2 +反应和肌动蛋白细胞骨架调节中发挥了作用。但是,它在调节TCR组分(包括ζ链,CD3δ,ε,γ链以及相关的激酶Lck和ZAP-70)的磷酸化中的功能尚不清楚。为了更全面地了解Vavl在受体近端叹气中的作用,我们在整个TCR刺激过程中,对VavI缺陷T细胞进行了定量蛋白质组学分析,对Vavl依赖性酪氨酸磷酸化事件进行了大规模表征。重要的是,这项研究揭示了Vav1在负反馈调节链,CD3δ,ε,γ链以及关键T细胞酪氨酸激酶Itk上的活化受体基于酪氨酸的活化基序的磷酸化中的新功能。 ,Lck和ZAP-70。我们的研究还发现了Vavl在CD28和TCR信号通路之间的串扰中以前没有被认识的作用。

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