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首页> 外文期刊>Frontiers in Immunology >T Cell Receptor (TCR)-Induced PLC-γ1 Sumoylation via PIASxβ and PIAS3 SUMO E3 Ligases Regulates the Microcluster Assembly and Physiological Function of PLC-γ1
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T Cell Receptor (TCR)-Induced PLC-γ1 Sumoylation via PIASxβ and PIAS3 SUMO E3 Ligases Regulates the Microcluster Assembly and Physiological Function of PLC-γ1

机译:T细胞受体(TCR)诱导的PIASxβ和PIAS3 SUMO E3 Ligases的PLC-γ1糖基化调节了PLC-γ1的微簇装配和生理功能

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The SUMO modification system plays an important role in T cell activation, yet how sumoylation regulates TCR-proximal signaling remains largely unknown. We show here that Phospholipase C-γ1 (PLC-γ1) is conjugated by SUMO1 at K54 and K987 upon TCR stimulation and that K54 sumoylation is pivotal for PLC-γ1-mediated T cell activation. We further demonstrate that TCR-induced K54 sumoylation of PLC-γ1 significantly promotes the formation of PLC-γ1 microclusters and the association of PLC-γ1 with the adaptor proteins SLP76 and Gads, but only slightly affects the phosphorylation of PLC-γ1 on Y783, which determines the enzyme catalytic activity. Moreover, upon TCR stimulation, the SUMO E3 ligases PIASxβ and PIAS3 both interact with PLC-γ1 and cooperate to sumoylate PLC-γ1, facilitating the assembly of PLC-γ1 microclusters. Together, our findings reveal a critical role of PLC-γ1 K54 sumoylation in PLC-γ1 microcluster assembly that controls PLC-γ1-mediated T cell activation, suggesting that sumoylation may have an important role in the microcluster assembly of TCR-proximal signaling proteins.
机译:SUMO修饰系统在T细胞活化中起着重要作用,但是,磺酰化如何调节TCR-近端信号转导仍然未知。我们在这里显示,磷脂酶C-γ1(PLC-γ1)在TCR刺激下被SUMO1在K54和K987处缀合,并且K54的磺酰化作用对于PLC-γ1介导的T细胞活化至关重要。我们进一步证明,TCR诱导的PLC-γ1K54磺酰化显着促进了PLC-γ1微簇的形成以及PLC-γ1与衔接蛋白SLP76和Gads的缔合,但对Y783上PLC-γ1的磷酸化影响很小,它决定了酶的催化活性。此外,在受到TCR刺激后,SUMO E3连接酶PIASxβ和PIAS3均与PLC-γ1相互作用,并协同合成PLC-γ1,从而促进了PLC-γ1微簇的组装。在一起,我们的发现揭示了PLC-γ1K54 sumoylation在控制PLC-γ1介导的T细胞活化的PLC-γ1微簇装配中的关键作用,表明sumoylation可能在TCR近端信号蛋白的微簇装配中具有重要作用。

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