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Toward Rational Design of Protein Detergent Complexes: Determinants of Mixed Micelles That Are Critical for the In Vitro Stabilization of a G-Protein Coupled Receptor

机译:迈向蛋白质洗涤剂复合物的合理设计:混合胶束的决定因素对G蛋白偶联受体的体外稳定化至关重要

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摘要

Although reconstitution of membrane proteins within protein detergent complexes is often used to enable their structural or biophysical characterization, it is unclear how one should rationally choose the appropriate micellar environment to preserve native protein folding. Here, we investigated model mixed micelles consisting of a nonionic glucosylated alkane surfactant from the maltoside and thiomaltoside families, bile salt surfactant, and the steryl derivative cholesteryl hemisuccinate. We correlated several key attributes of these micelles with the in vitro ligand-binding activity of hA2aR in these systems. Through small-angle neutron scattering and radioligand-binding analysis, we found several key aspects of mixed micellar systems that preserve the activity of hA2aR, including a critical amount of cholesteryl hemisuccinate per micelle, and an optimal hydrophobic thickness of the micelle that is analogous to the thickness of native mammalian bilayers. These features are closely linked to the headgroup chemistry of the surfactant and the hydrocarbon chain length, which influence both the morphology and composition of resulting micelles. This study should serve as a general guide for selecting the appropriate mixed surfactant systems to stabilize membrane proteins for biophysical analysis.
机译:尽管通常使用蛋白去污剂复合物中的膜蛋白重构来实现其结构或生物物理表征,但尚不清楚如何合理选择合适的胶束环境来保留天然蛋白折叠。在这里,我们研究了由麦芽糖苷和硫代麦芽糖苷家族的非离子型糖基化烷烃表面活性剂,胆盐表面活性剂和甾醇衍生物胆固醇半琥珀酸酯组成的混合胶束模型。我们将这些胶束的几个关键属性与hA2aR在这些系统中的体外配体结合活性相关联。通过小角度中子散射和放射性配体结合分析,我们发现了保留hA2aR活性的混合胶束系统的几个关键方面,包括每个胶束临界量的胆固醇半琥珀酸酯以及与该胶束相似的最佳疏水厚度原生哺乳动物双层的厚度。这些特征与表面活性剂的头基化学性质和烃链长度密切相关,后者影响所得胶束的形态和组成。该研究应作为选择合适的混合表面活性剂体系以稳定膜蛋白进行生物物理分析的一般指南。

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