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首页> 外文期刊>Molecular biology of the cell >Organization of the integrin LFA-1 in nanoclusters regulates its activity
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Organization of the integrin LFA-1 in nanoclusters regulates its activity

机译:整群蛋白LFA-1在纳米簇中的组织调节其活性

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摘要

The beta 2-integrin LFA-1 facilitates extravasation of monocytes (MOs) into the underlying tissues, where MOs can differentiate into dendritic cells (DCs). Although DCs express LFA-1, unlike MOs, they cannot bind to ICAM-1. We hypothesized that an altered integrin organization on the DC plasma membrane might cause this effect and investigated the relationship between membrane organization and function of LFA-1 on MOs and DCs. High-resolution mapping of LFA-1 surface distribution revealed that on MOs LFA-1 function is associated with a distribution in well-defined nanoclusters (100-150-nm diameter). Interestingly, a fraction of these nanoclusters contains primed LFA-1 molecules expressing the specific activation-dependent L16-epitope. Live imaging of MO-T-cell conjugates showed that only these primed nanoclusters are dynamically recruited to the cellular interface forming micrometer-sized assemblies engaged in ligand binding and linked to talin. We conclude that besides affinity regulation, LFA-1 function is controlled by at least three different avidity patterns: random distributed inactive molecules, well-defined ligand-independent proactive nanoclusters, and ligand-triggered micrometer-sized macroclusters.
机译:β2-整合素LFA-1促进单核细胞(MOs)外渗到基础组织中,在这些组织中MOs可以分化为树突状细胞(DCs)。尽管DC表达LFA-1,但与MO不同,它们不能与ICAM-1结合。我们假设,DC质膜上整合素组织的改变可能会引起这种作用,并研究了LFA-1在MOs和DCs上的膜组织与功能之间的关系。 LFA-1表面分布的高分辨率映射显示,在MOs上,LFA-1功能与明确定义的纳米团簇(直径为100-150 nm)中的分布有关。有趣的是,这些纳米簇中的一小部分包含表达特定活化依赖性L16表位的引发的LFA-1分子。 MO-T细胞缀合物的实时成像显示,只有这些涂有底漆的纳米簇被动态募集到细胞界面,形成参与配体结合并与塔林素连接的微米级组件。我们得出的结论是,除了亲和力调节外,LFA-1的功能还受至少三种不同的亲和力模式控制:随机分布的无活性分子,定义明确的不依赖配体的活性纳米簇和配体触发的微米级宏观簇。

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