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Differential Impact of Caveolae and Caveolin-1 Scaffolds on The Membrane Raft Proteome

机译:Caveolae和Caveolin-1支架对膜筏蛋白质组的差异影响。

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摘要

Caveolae, a class of cholesterol-rich lipid rafts, are smooth invaginations of the plasma membrane whose formation in nonmuscle cells requires caveolin-1 (Cav1). The recent demonstration that Cav1-associated cavin proteins, in particular PTRF/cavin-1, are also required for caveolae formation supports a functional role for Cav1 independently of caveolae. In tumor cells deficient for Golgi β-1,6N-acetylglucosaminyltransferase V (Mgat5), reduced Cav1 expression is associated not with caveolae but with oligomerized Cav1 domains, or scaffolds, that functionally regulate receptor signaling and raft-dependent endocytosis. Using subdiffraction-limit microscopy, we show that Cav1 scaffolds are homogenous subdiffraction-limit sized structures whose size distribution differs from that of Cav1 in caveolae expressing cells. These cell lines displaying differing Cav1/caveolae phenotypes are effective tools for probing the structure and composition of caveolae. Using stable isotope labeling by amino acids in cell culture, we are able to quantitatively distinguish the composition of caveolae from the background of detergent-resistant membrane proteins and show that the presence of caveolae enriches the protein composition of detergent-resistant membrane, including the recruitment of multiple heterotrimeric G-protein subunits. These data were further supported by analysis of immuno-isolated Cav1 domains and of methyl-β-cyclodextrin-disrupted detergent-resistant membrane. Our data show that loss of caveolae results in a dramatic change to the membrane raft proteome and that this change is independent of Cav1 expression. The proteomics data, in combination with subdiffraction-limit microscopy, indicates that noncaveolar Cav1 domains, or scaffolds are structurally and functionally distinct from caveolae and differentially impact on the molecular composition of lipid rafts.
机译:Caveolae是一类富含胆固醇的脂质筏,是质膜的平滑内陷,其在非肌肉细胞中的形成需要Caveolin-1(Cav1)。最近的证明Cav1相关cavin蛋白,特别是PTRF / cavin-1,也是小窝形成所必需的,这支持了Cav1的功能作用,独立于小窝。在缺乏高尔基体β-1,6N-乙酰氨基葡萄糖氨基转移酶V(Mgat5)的肿瘤细胞中,降低的Cav1表达与小窝无关,而是与功能性调节受体信号传导和筏依赖性内吞作用的寡聚Cav1域或支架相关。使用亚衍射极限显微镜,我们显示Cav1支架是同质亚衍射极限大小的结构,其大小分布与表达caveolae的细胞中的Cav1不同。这些显示不同的Cav1 / caveolae表型的细胞系是探测小窝结构和组成的有效工具。在细胞培养中使用氨基酸进行稳定的同位素标记,我们能够从耐去污剂的膜蛋白背景上定量区分小窝的组成,并表明小窝的存在丰富了耐洗剂的膜的蛋白质组成,包括募集多个异三聚体G蛋白亚基的组成。通过免疫分离的Cav1结构域和甲基-β-环糊精破坏的去污剂抗性膜的分析进一步支持了这些数据。我们的数据表明,海绵体的丢失导致膜筏蛋白质组发生了巨大变化,并且这种变化与Cav1表达无关。蛋白质组学数据与亚衍射极限显微镜结合表明,非小窝Cav1结构域或支架在结构和功能上与小窝不同,并且对脂质筏的分子组成有不同的影响。

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