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Distinct Kinetics Features of LFA-1 and Mac-1 in Neutrophil Activation

机译:LFA-1和Mac-1在嗜中性粒细胞活化中的独特动力学特征

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LFA-1 and Mac-1, two p2 integrin members constitutively expressed on neutrophils, mediate leukocyte recruitment cascade by binding to the same ligand of ICAM-1. The slow rolling and firm adhesion of leukocytes rely on LFA-1 while the cell crawling is dependent on Mac-1. We hypothesized that their distinct roles are likely attributed to the differences in the binding kinetics or in the diverse responses of outside-in and inside-out signaling. In this study, we compared the ICAM-1 binding features between soluble or membrane-expressed LFA-1 and Mac-1 with different affinity conformation using optical trap technique. Our data indicated that the affinity up-regulation from wide type (WT) to high affinity (HA) is off-rate dependent for LFA-1 but on-rate dependent for Mac-1. The structural bases of this new finding were found to be consistent with our previous simulations. These results furthered our understanding in their function differences under shear flow.
机译:LFA-1和Mac-1,在中性粒细胞上组成性表达的两个p2整合素成员,通过与ICAM-1的同一配体结合,介导白细胞募集级联。白细胞的缓慢滚动和牢固的粘附依赖于LFA-1,而细胞爬行则依赖于Mac-1。我们假设它们的独特作用可能归因于结合动力学的差异或由外而内和由内而外的信号传导的不同反应。在这项研究中,我们使用光阱技术比较了具有不同亲和力构象的可溶性或膜表达的LFA-1和Mac-1之间的ICAM-1结合特征。我们的数据表明,从宽型(WT)到高亲和力(HA)的亲和力上调与LFA-1的速率无关,而对Mac-1则与速率有关。发现这一新发现的结构基础与我们先前的模拟是一致的。这些结果使我们进一步了解了剪切流作用下它们的功能差异。

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