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首页> 外文期刊>Nature Communications >Dual functions of Rap1 are crucial for T-cell homeostasis and prevention of spontaneous colitis
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Dual functions of Rap1 are crucial for T-cell homeostasis and prevention of spontaneous colitis

机译:Rap1的双重功能对于T细胞稳态和预防自发性结肠炎至关重要

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Rap1-GTP activates leukocyte function-associated antigen-1 (LFA-1) to induce arrest on the high endothelial venule (HEV). Here we show that Rap1-GDP restrains rolling behaviours of T cells on the peripheral lymph node addressin (PNAd), P-selectin and mucosal addressin cell adhesion molecule-1 (MadCAM-1) by inhibiting tether formation. Consequently, Rap1 deficiency impairs homing of naive T cells to peripheral lymph nodes, but accelerates homing of T(H)17 and T(H)1 cells to the colon, resulting in spontaneous colitis with tumours. Rap1-GDP associates with and activates lymphocyte-oriented kinase, which phosphorylates ERM (ezrin, radixin and moesin) in resting T cells. Phosphomimetic ezrin reduces the rolling of Rap1-deficient cells, and thereby decreases their homing into the colon. On the other hand, chemokines activate Rap1 at the plasma membrane within seconds, and Rap1-GTP binds to filamins, which diminishes its association with the beta(2) chain of LFA-1 and results in LFA-1 activation. This Rap1-dependent regulation of T-cell circulation prevents the onset of colitis.
机译:Rap1-GTP激活白细胞功能相关抗原1(LFA-1),以诱导在高内皮小静脉(HEV)上的停滞。在这里,我们显示Rap1-GDP通过抑制系链的形成来抑制T细胞在周围淋巴结地址蛋白(PNAd),P选择素和粘膜地址蛋白细胞粘附分子1(MadCAM-1)上的滚动行为。因此,Rap1缺乏会损害幼稚T细胞向外周淋巴结的归巢,但会加速T(H)17和T(H)1细胞向结肠的归巢,从而导致具有肿瘤的自发性结肠炎。 Rap1-GDP与淋巴细胞定向激酶相关并活化,该激酶使静止T细胞中的ERM(ezrin,radixin和moesin)磷酸化。拟磷酸化ezrin减少了Rap1缺陷细胞的滚动,从而减少了它们归巢到结肠中的过程。另一方面,趋化因子在几秒钟内激活质膜上的Rap1,Rap1-GTP与丝素结合,从而减弱了它与LFA-1的beta(2)链的结合并导致LFA-1激活。 T细胞循环的这种Rap1依赖性调节可防止结肠炎的发作。

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