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Technical Advance: Changes in neutrophil migration patterns upon contact with platelets in a microfluidic assay

机译:技术进步:在微流分析中接触血小板后嗜中性粒细胞迁移模式的变化

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摘要

Neutrophils are traditionally regarded as the "first responders" of the immune system. However, recent observations revealed that platelets often respond earlier to recruit and activate neutrophils within sites of injury and inflammation. Currently, platelet–neutrophil interactions are studied by intravital microscopy. Although such studies provide exceptional, physiologic in vivo data, they are also laborious and have low throughput. To accelerate platelet–neutrophil interaction studies, we have developed and optimized an ex vivo microfluidic platform with which the interactions between platelets and moving neutrophils are measured at single-cell level in precise conditions and with high throughput. With the use of this new assay, we have evaluated changes in neutrophil motility upon direct contact with platelets. Motility changes include longer distances traveled, frequent changes in direction, and faster neutrophil velocities compared with a standard motility response to chemoattractant fMLP. We also found that the neutrophil–platelet direct interactions are transient and mediated by CD62P–CD162 interactions, localized predominantly at the uropod of moving neutrophils. This "crawling," oscillatory neutrophil behavior upon platelet contact is consistent with previous in vivo studies and validates the use of this new test for the exploration of this interactive relationship.
机译:传统上,嗜中性粒细胞被视为免疫系统的“第一反应者”。然而,最近的观察表明,血小板通常在损伤和炎症部位较早响应以募集并激活嗜中性粒细胞。目前,通过活体显微镜研究了血小板与中性粒细胞的相互作用。尽管此类研究提供了出色的体内生理数据,但它们也费力且通量低。为了加快血小板与中性粒细胞相互作用的研究,我们开发并优化了体外微流体平台,利用该平台可以在精确条件下以高通量在单细胞水平上测量血小板与运动性中性粒细胞之间的相互作用。通过使用这种新的检测方法,我们评估了直接接触血小板后嗜中性粒细胞运动的变化。与标准趋化性对化学引诱剂fMLP的反应相比,运动性改变包括行进的距离更长,方向频繁变化以及中性粒细胞的速度更快。我们还发现,中性粒细胞与血小板的直接相互作用是短暂的,并由CD62P-CD162相互作用介导,主要定位于运动中性粒细胞的尾足。血小板接触后这种“爬行”的中性粒细胞振荡行为与先前的体内研究一致,并验证了这种新方法在探索这种相互作用关系中的应用。

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