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Integrin-mediated adhesion regulates membrane order

机译:整合素介导的粘附调节膜秩序

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摘要

The properties of cholesterol-dependent domains (lipid rafts) in cell membranes have been controversial. Because integrin-mediated cell adhesion and caveolin both regulate trafficking of raft components, we investigated the effects of adhesion and caveolin on membrane order. The fluorescent probe Laurdan and two-photon microscopy revealed that focal adhesions are highly ordered; in fact, they are more ordered than caveolae or domains that stain with cholera toxin subunit B (CtxB). Membrane order at focal adhesion depends partly on phosphorylation of caveolin1 at Tyr14, which localizes to focal adhesions. Detachment of cells from the substratum triggers a rapid, caveolin-independent decrease in membrane order, followed by a slower, caveolin-dependent decrease that correlates with internalization of CtxB-stained domains. Endocytosed CtxB domains also become more fluid. Thus, membrane order is highly dependent on caveolae and focal adhesions. These results show that lipid raft properties are conferred by assembly of specific protein complexes. The ordered state within focal adhesions may have important consequences for signaling at these sites.
机译:细胞膜中胆固醇依赖性结构域(脂质筏)的性质一直存在争议。由于整联蛋白介导的细胞粘附和caveolin都调节筏组件的运输,我们研究了粘附和caveolin对膜顺序的影响。荧光探针劳尔丹(Laurdan)和双光子显微镜显示,粘着斑高度有序。实际上,它们比被霍乱毒素亚基B(CtxB)染色的小窝或结构域更有序。粘着斑处的膜顺序部分取决于Tyr14处caveolin1的磷酸化,其定位于粘着斑。细胞从基质中脱离会触发膜顺序的快速,不依赖caveolin的减少,然后触发较慢的caveolin依赖的减少,与CtxB染色域的内在化相关。内吞的CtxB结构域也变得更加流畅。因此,膜的顺序高度依赖于小孔和粘着斑。这些结果表明脂质筏的性质是由特定蛋白质复合物的组装赋予的。粘着斑内的有序状态可能会对这些部位的信号传导产生重要影响。

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