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The Rap1-RIAM-talin axis of integrin activation and blood cell function

机译:Rap1-RIAM-talin整合素激活和血细胞功能轴

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摘要

Integrin adhesion receptors mediate the adhesion of blood cells, such as leukocytes, to other cells, such as endothelial cells. Integrins also are critical for anchorage of hematopoietic precursors to the extracellular matrix. Blood cells can dynamically regulate the affinities of integrins for their ligands ("activation"), an event central to their functions. Here we review recent progress in understanding the mechanisms of integrin activation with a focus on the functions of blood cells. We discuss how talin binding to the integrin beta cytoplasmic domain, in conjunction with the plasma membrane, induces long-range allosteric rearrangements that lead to integrin activation. Second, we review our understanding of how signaling events, particularly those involving Rap1 small guanosine triphosphate (GTP) hydrolases, can regulate the talin-integrin interaction and resulting activation. Third, we review recent findings that highlight the role of the Rap1-GTP-interacting adapter molecule (RIAM), encoded by the APBB1IP gene, in leukocyte integrin activation and consequently in leukocyte trafficking.
机译:整联蛋白粘附受体介导血细胞(例如白细胞)与其他细胞(例如内皮细胞)的粘附。整联蛋白对于将造血前体锚定到细胞外基质上也至关重要。血细胞可以动态调节整联蛋白对其配体的亲和力(“激活”),这是对其功能至关重要的事件。在这里,我们回顾了了解整联蛋白激活机制的最新进展,重点是血细胞的功能。我们讨论如何talin绑定到整联蛋白β胞质域,与质膜结合,诱导导致整联蛋白激活的远程变构重排。第二,我们回顾我们对信号事件,尤其是涉及Rap1小鸟苷三磷酸(GTP)水解酶的信号事件如何调节塔林-整合素相互作用和激活的理解。第三,我们回顾了最近的发现,这些发现突出了由APBB1IP基因编码的Rap1-GTP相互作用适配器分子(RIAM)在白细胞整合素激活中的作用,并因此在白细胞运输中的作用。

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