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Molecular Characterization of Caveolin-induced Membrane Curvature

机译:卡夫林诱导的膜曲率的分子表征

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摘要

The generation of caveolae involves insertion of the cholesterol-binding integral membrane protein caveolin-1 (Cav1) into the membrane, however, the precise molecular mechanisms are as yet unknown. We have speculated that insertion of the caveolin scaffolding domain (CSD), a conserved amphipathic region implicated in interactions with signaling proteins, is crucial for caveola formation. We now define the core membrane-juxtaposed region of Cav1 and show that the oligomerization domain and CSD are protected by tight association with the membrane in both mature mammalian caveolae and a model prokaryotic system for caveola biogenesis. Cryoelectron tomography reveals the core membrane-juxtaposed domain to be sufficient to maintain oligomerization as defined by polyhedral distortion of the caveolar membrane. Through mutagenesis we demonstrate the importance of the membrane association of the oligomerization domain/CSD for defined caveola biogenesis and furthermore, highlight the functional significance of the intramembrane domain and the CSD for defined caveolin-induced membrane deformation. Finally, we define the core structural domain of Cav1, constituting only 66 amino acids and of great potential to nanoengineering applications, which is required for caveolin-induced vesicle formation in a bacterial system. These results have significant implications for understanding the role of Cav1 in caveola formation and in regulating cellular signaling events.
机译:小窝的产生涉及将结合胆固醇的整合膜蛋白小窝蛋白-1(Cav1)插入膜中,但是,确切的分子机制尚不清楚。我们推测小窝支架结构域(CSD)的插入,一个保守的两亲性区域牵连与信号蛋白的相互作用,对小窝形成至关重要。现在,我们定义了Cav1的核心膜并置区域,并表明寡聚化域和CSD通过与膜紧密结合而受到保护,在成熟的哺乳动物小窝和小窝生物发生的模型原核系统中。低温电子断层扫描显示核心膜并置域足以维持寡聚化,如由海绵膜的多面体形变所定义。通过诱变,我们证明了寡聚化域/ CSD的膜缔合对于确定的caveola生物发生的重要性,此外,突出了膜内域和CSD对确定的caveolin诱导的膜变形的功能意义。最后,我们定义了Cav1的核心结构域,仅构成66个氨基酸,具有纳米工程应用的巨大潜力,这是caveolin诱导细菌系统中囊泡形成所需的。这些结果对于理解Cav1在小窝形成和调控细胞信号事件中的作用具有重要意义。

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