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Cells on the run: shear regulated integrin activation in leukocyte rolling and arrest on endothelial cells

机译:运行中的细胞:剪切调节整白蛋白在白细胞滚动中的活化并停滞在内皮细胞上

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摘要

The arrest of rolling leukocytes on various target vascular beds is mediated by specialized leukocyte integrins and their endothelial immunoglobulin superfamily (IgSF) ligands. These integrins are kept in largely inactive states and undergo in situ activation upon leukocyte-endothelial contact by both biochemical and mechanical signals from flow-derived shear forces. In vivo and in vitro studies suggest that leukocyte integrin activation involves conformational alterations through inside-out signaling followed by ligand-induced rearrangements accelerated by external forces. This activation process takes place within fractions of seconds by in situ signals transduced to the rolling leukocyte as it encounters specialized endothelial-displayed chemoattractants, collectively termed arrest chemokines. In neutrophils, selectin rolling engagements trigger intermediate affinity integrins to support reversible adhesions prior to chemokine triggered arrest. Different leukocyte subsets appear to use different modalities of integrin activation during rolling and arrest at distinct endothelial sites.
机译:滚动白细胞在各种靶血管床上的停滞是由专门的白细胞整合素及其内皮免疫球蛋白超家族(IgSF)配体介导的。这些整联蛋白保持在很大程度上不活泼的状态,并在白细胞-内皮接触时通过来自流动的剪切力的生化和机械信号进行原位活化。体内和体外研究表明,白细胞整联蛋白活化涉及通过内外信号传导进行构象改变,然后由外力加速配体诱导的重排。当激活的白细胞遇到专门的内皮展示的趋化因子(统称为停滞趋化因子)时,其激活过程在几分之一秒内就被原位信号传递给滚动的白细胞。在嗜中性粒细胞中,选择素滚动接合在趋化因子触发停滞之前触发中间亲和力整联蛋白以支持可逆粘附。不同的白细胞亚群似乎在滚动和停滞在不同的内皮部位时使用了不同的整合素激活方式。

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