首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Cdc42 regulates neutrophil migration via crosstalk between WASp, CD11b, and microtubules
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Cdc42 regulates neutrophil migration via crosstalk between WASp, CD11b, and microtubules

机译:Cdc42通过WASp,CD11b和微管之间的串扰调节嗜中性粒细胞迁移

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Chemotaxis promotes neutrophil participation in cellular defense by enabling neutrophil migration to infected tissue and is controlled by persistent cell polarization. One long-standing question of neutrophil polarity has been how the pseudopod and the uropod are coordinated. In our previous report, we suggested that Rho GTPase Cdc42 controls neutrophil polarity through CD11b signaling at the uropod, albeit through an unknown mechanism. Here, we show that Cdc42 controls polarity, unexpectedly, via its effector WASp. Cdc42 controls WASp activation and its distant localization to the uropod. At the uropod, WASp regulates the reorganization of CD11b integrin into detergent resistant membrane domains; in turn, CD11b recruits the microtubule end binding protein EB1 to capture and stabilize microtubules at the uropod. This organization is necessary to maintain neutrophil polarity during migration and is critical for neutrophil emigration into inflamed lungs. These results suggest unrecognized mechanism of neutrophil polarity in which WASp mediates long-distance control of the uropod by Cdc42 to maintain a proper balance between the pseudopod and the uropod. Our study reveals a new function for WASp in the control of neutrophil polarity via crosstalk between CD11b and microtubules.
机译:趋化性通过使嗜中性粒细胞迁移到感染组织而促进嗜中性粒细胞参与细胞防御,并受持续的细胞极化作用的控制。中性粒细胞极性的一个长期存在的问题是假足和尾足如何协调。在我们以前的报告中,我们建议Rho GTPase Cdc42通过在uropod上的CD11b信号传导控制嗜中性粒细胞极性,尽管是通过未知的机制。在这里,我们展示了Cdc42意外地通过其效应器WASp控制极性。 Cdc42控制WASp的激活及其对尾足的远距离定位。在尾足处,WASp调节CD11b整联蛋白重组为抗洗涤剂的膜结构域。反过来,CD11b募集微管末端结合蛋白EB1,以捕获并稳定尾足上的微管。该组织对于在迁移过程中维持嗜中性粒细胞极性是必不可少的,对于嗜中性粒细胞迁移到发炎的肺部至关重要。这些结果提示了中性粒细胞极性的无法识别的机制,其中WASp通过Cdc42介导了对uropod的长距离控制,以维持假足和uropod之间的适当平衡。我们的研究揭示了WASp通过CD11b和微管之间的串扰控制嗜中性粒细胞极性的新功能。

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