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Molecular Rheology of Neuronal Membranes Explored using A Molecular Rotor: Implications for Receptor Function

机译:使用分子转子探索神经元膜的分子流变学:受体功能的含义。

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摘要

Abstract The role of membrane cholesterol as a crucial regulator in the structure and function of membrane proteins and receptors is well documented. However, there is a lack of consensus on the mechanism for such regulation. We have previously shown that the function of an important neuronal receptor, the serotonin1A receptor, is modulated by cholesterol in hippocampal membranes. With an overall objective of addressing the role of membrane physical properties in receptor function, we measured the viscosity of hippocampal membranes of varying cholesterol content using a meso-substituted fluorophore (BODIPY-C12) based on the BODIPY probe. BODIPY-C12 acts as a fluorescent molecular rotor and allows measurement of hippocampal membrane viscosity through its characteristic viscosity-sensitive fluorescence depolarization. A striking feature of our results is that specific agonist binding by the serotonin1A receptor exhibits close correlation with hippocampal membrane viscosity, implying the importance of global membrane properties in receptor function. We envision that our results are important in understanding GPCR regulation by the membrane environment, and is relevant in the context of diseases in which GPCR signaling plays a major role and are characterized by altered membrane fluidity.
机译:摘要膜胆固醇在膜蛋白和受体的结构和功能中起着至关重要的调节作用。但是,对于这种监管机制尚缺乏共识。先前我们已经表明,重要的神经元受体5-羟色胺1A受体的功能受到海马膜中胆固醇的调节。为了解决膜物理特性在受体功能中的作用的总体目标,我们使用基于BODIPY探针的内消旋荧光团(BODIPY-C12)测量了胆固醇含量不同的海马膜的粘度。 BODIPY-C12充当荧光分子转子,并通过其特有的粘度敏感型荧光去极化功能来测量海马膜粘度。我们结果的一个显着特征是血清素1A受体与特定激动剂的结合表现出与海马膜粘度的密切相关,这暗示着全局膜特性对受体功能的重要性。我们设想我们的结果对于理解膜环境对GPCR的调控非常重要,并且在以GPCR信号起主要作用并以膜流动性改变为特征的疾病中也具有重要意义。

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