首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Cutting Edge: Fyn Is Essential for Tyrosine Phosphorylation of Csk-Binding Protein/Phosphoprotein Associated with Glycolipid-Enriched Microdomains in Lipid Rafts in Resting T Cells.
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Cutting Edge: Fyn Is Essential for Tyrosine Phosphorylation of Csk-Binding Protein/Phosphoprotein Associated with Glycolipid-Enriched Microdomains in Lipid Rafts in Resting T Cells.

机译:前沿:Fyn是与静止的T细胞中脂筏中富含糖脂的微域相关的Csk结合蛋白/磷酸酪氨酸磷酸化所必需的。

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摘要

In resting T cells, Csk is constitutively localized in lipid rafts by virtue of interaction with a phosphorylated adaptor protein, Csk-binding protein (Cbp)/phosphoprotein associated with glycolipid-enriched microdomains, and sets an activation threshold in TCR signaling. In this study, we examined a kinase responsible for Cbp phosphorylation in T cell membrane rafts. By analyzing T cells from Fyn(-/-) mice, we clearly demonstrated that Fyn, but not Lck, has its kinase activity in membrane rafts, and plays a critical role in Cbp phosphorylation, Cbp-Csk interaction, and Csk kinase activity. Naive CD44(low)CD62 ligand(high) T cells were substantially reduced in Fyn(-/-) mice, presumably due to the inhibition of Cbp phosphorylation. Thus, Fyn mediates Cbp-Csk interaction and recruits Csk to rafts by phosphorylating Cbp. Csk recruited to rafts would then be activated and inhibit the kinase activity of Lck to keep resting T cells in a quiescent state. Our results elucidate a negative regulatory role for Fyn in proximal TCR signaling in lipid rafts.
机译:在静止的T细胞中,Csk通过与磷酸化的衔接蛋白,与富含糖脂的微域相关的Csk结合蛋白(Cbp)/磷酸蛋白相互作用而在脂质筏中组成性地定位,并在TCR信号传导中设置激活阈值。在这项研究中,我们检查了负责T细胞膜筏中Cbp磷酸化的激酶。通过分析来自Fyn(-/-)小鼠的T细胞,我们清楚地证明Fyn(而非Lck)在膜筏中具有其激酶活性,并且在Cbp磷酸化,Cbp-Csk相互作用和Csk激酶活性中起关键作用。幼稚的CD44(低)CD62配体(高)T细胞在Fyn(-/-)小鼠中显着减少,可能是由于抑制了Cbp磷酸化。因此,Fyn介导Cbp-Csk相互作用,并通过磷酸化Cbp将Csk募集到木筏中。然后募集到木筏中的Csk将被激活并抑制Lck的激酶活性,从而使静止的T细胞保持静止状态。我们的结果阐明了Fyn在脂质筏中近端TCR信号传导中的负调控作用。

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