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Local microvascular leakage promotes trafficking of activated neutrophils to remote organs

机译:局部微血管泄漏促进将活化中性粒细胞的贩运到远程器官

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Increased microvascular permeability to plasma proteins and neutrophil emigration are hallmarks of innate immunity and key features of numerous inflammatory disorders. Although neutrophils can promote microvascular leakage, the impact of vascular permeability on neutrophil trafficking is unknown. Here, through the application of confocal intravital microscopy, we report that vascular permeability–enhancing stimuli caused a significant frequency of neutrophil reverse transendothelial cell migration (rTEM). Furthermore, mice with a selective defect in microvascular permeability enhancement ( VEC-Y685F-ki ) showed reduced incidence of neutrophil rTEM. Mechanistically, elevated vascular leakage promoted movement of interstitial chemokines into the bloodstream, a response that supported abluminal-to-luminal neutrophil TEM. Through development of an in vivo cell labeling method we provide direct evidence for the systemic dissemination of rTEM neutrophils, and showed them to exhibit an activated phenotype and be capable of trafficking to the lungs where their presence was aligned with regions of vascular injury. Collectively, we demonstrate that increased microvascular leakage reverses the localization of directional cues across venular walls, thus causing neutrophils engaged in diapedesis to reenter the systemic circulation. This cascade of events offers a mechanism to explain how local tissue inflammation and vascular permeability can induce downstream pathological effects in remote organs, most notably in the lungs.
机译:对血浆蛋白质和中性粒细胞移民的显微血管渗透性增加是先天免疫的标志和许多炎症障碍的关键特征。虽然中性粒细胞可以促进微血管泄漏,但血管渗透性对中性粒细胞贩运的影响是未知的。在这里,通过占用腔内显微镜的应用,我们报告了血管渗透性增强刺激导致中性粒细胞逆转脑细胞迁移(RTEM)的显着频率。此外,微血管渗透性增强中具有选择性缺陷的小鼠(VEC-Y685F-Ki)显示出中性粒细胞RTEM的发病率降低。机械地,升高的血管泄漏促进间质趋化因子的运动进入血液流入血液中,一种负载抑形对腔中性粒细胞TEM的反应。通过在体内细胞标记方法的发展中,我们为RTEM中性粒细胞的全身传播提供直接证据,并显示它们表现出活化表型并能够贩运其存在与血管损伤区域对齐的肺部。总的来说,我们证明了微血管泄漏增加逆转旋转壁的定位方向性提示的定位,从而导致从事粘性作用的中性粒细胞再入系统循环。这种级联的事件提供了一种解释局部组织炎症和血管渗透性如何在偏远器官中诱导局部病理局部的机制,最值得注意的是肺部。

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