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首页> 外文期刊>Nature Communications >Tespa1 regulates T cell receptor-induced calcium signals by recruiting inositol 1,4,5-trisphosphate receptors
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Tespa1 regulates T cell receptor-induced calcium signals by recruiting inositol 1,4,5-trisphosphate receptors

机译:Tespa1通过募集肌醇1,4,5-三磷酸受体来调节T细胞受体诱导的钙信号

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摘要

Thymocyte-expressed, positive selection-associated 1 (Tespa1) is important in T cell receptor (TCR)-driven thymocyte development. Downstream of the TCR, Tespa1 is a crucial component of the linker for activation of T cells (LAT) signalosome, facilitating calcium signalling and subsequent MAPK activation. However, it is unknown how Tespa1 elicits calcium signalling. Here, we show that inositol 1,4,5-trisphosphate receptor type 1 (IP3R1) is crucial for Tespa1-optimized, TCR-induced Ca2+ flux and thymocyte development. Upon TCR stimulation, Tespa1 directly interacts with IP3R1 and recruits it to the TCR complex, where IP3R1 is phosphorylated at Y353 by Fyn. This Tespa1-IP3R1 interaction is mediated by the F187 and F188 residues of Tespa1 and the amino-terminus of IP3R1. Tespa1-F187A/F188A mutant mice phenocopy Tespa1-deficient mice with impaired late thymocyte development due to reduced IP3R1 translocation to the TCR-proximal region. Our work elucidates the function of Tespa1 in T cell development and the regulation of TCR-induced Ca2+ signalling through IP3R1.
机译:胸腺细胞表达,正选择相关1(Tespa1)在T细胞受体(TCR)驱动的胸腺细胞发育中很重要。在TCR的下游,Tespa1是激活T细胞(LAT)信号小体,促进钙信号传导和随后MAPK激活的连接子的关键组成部分。但是,尚不清楚Tespa1如何引起钙信号传导。在这里,我们表明1型肌醇1,4,5-三磷酸受体(IP3R1)对于Tespa1优化,TCR诱导的Ca 2 + 通量和胸腺细胞发育至关重要。在受到TCR刺激后,Tespa1直接与IP3R1相互作用并将其募集到TCR复合物中,在IPR3处,Fyn将IP3R1磷酸化。 Tespa1-IP3R1的这种相互作用是由Tespa1的F187和F188残基以及IP3R1的氨基端介导的。 Tespa1-F187A / F188A突变小鼠的表型由于IP3R1向TCR-近端区域的转运减少,导致晚期胸腺细胞发育受损的Tespa1缺陷小鼠。我们的工作阐明了Tespa1在T细胞发育中的功能以及通过IP3R1调控TCR诱导的Ca 2 + 信号传导。

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