首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Rap1 controls lymphocyte adhesion cascade and interstitial migration within lymph nodes in RAPL-dependent and -independent manners.
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Rap1 controls lymphocyte adhesion cascade and interstitial migration within lymph nodes in RAPL-dependent and -independent manners.

机译:Rap1以RAPL依赖性和非依赖性方式控制淋巴结内的淋巴细胞粘附级联和间质迁移。

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摘要

The small GTPase Rap1 and its effector RAPL regulate lymphocyte adhesion and motility. However, their precise regulatory roles in the adhesion cascade preceding entry into lymph nodes and during interstitial migration are unclear. Here, we show that Rap1 is indispensably required for the chemokine-triggered initial arrest step of rolling lymphocytes through LFA-1, whereas RAPL is not involved in rapid arrest. RAPL and talin play a critical role in stabilizing lymphocyte arrest to the endothelium of blood vessels under flow or to the high endothelial venules of peripheral lymph nodes in vivo. Further, mutagenesis and peptide studies suggest that release of a trans-acting restraint from the beta2 cytoplasmic region of LFA-1 is critical for Rap1-dependent initial arrest. Rap1 or RAPL deficiency severely impaired lymphocyte motility over lymph node stromal cells in vitro, and RAPL deficiency impaired high-velocity directional movement within lymph nodes. These findings reveal the several critical steps of Rap1, which are RAPL-dependent and -independent, in lymphocyte trafficking.
机译:小的GTPase Rap1及其效应物RAPL调节淋巴细胞的粘附和运动。然而,它们在进入淋巴结之前和间质迁移过程中的粘附级联中的确切调控作用尚不清楚。在这里,我们显示Rap1是通过LFA-1滚动淋巴细胞的趋化因子触发的初始停滞步骤必不可少的,而RAPL不参与快速停滞。 RAPL和他林在稳定淋巴细胞在流动中对血管内皮的阻滞或对体内外周淋巴结的高内皮微静脉起关键作用。此外,诱变和多肽研究表明,从LFA-1的β2细胞质区域释放反式抑制因子对于依赖Rap1的初始逮捕至关重要。 Rap1或RAPL缺乏严重损害了体外淋巴结间质细胞的淋巴细胞运动,而RAPL缺乏损害了淋巴结内的高速定向运动。这些发现揭示了Rap1在淋巴细胞运输中的几个关键步骤,这些步骤是RAPL依赖性和非依赖性的。

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