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蛋白质结合对脂质侧向流动性和膜相结构的调节作用。

Lipid lateral mobility and membrane phase structure modulation by protein binding.

作者信息

Forstner Martin B, Yee Chanel K, Parikh Atul N, Groves Jay T

机构信息

Department of Chemistry, University of California, Berkeley, California 94720, USA.

出版信息

J Am Chem Soc. 2006 Nov 29;128(47):15221-7. doi: 10.1021/ja064093h.

Abstract

Using a combination of fluorescence correlation and infrared absorption spectroscopies, we characterize lipid lateral diffusion and membrane phase structure as a function of protein binding to the membrane surface. In a supported membrane configuration, cholera toxin binding to the pentasaccharaide headgroup of membrane-incorporated GM1 lipid alters the long-range lateral diffusion of fluorescently labeled probe lipids, which are not involved in the binding interaction. This effect is prominently amplified near the gel-fluid transition temperature, Tm, of the majority lipid component. At temperatures near Tm, large changes in probe lipid diffusion are measured at average protein coverage densities as low as 0.02 area fraction. Spectral shifts of the methylene symmetric and asymmetric stretching modes in the lipid acyl chain confirm that protein binding alters the fraction of lipid in the gel phase.

摘要

我们结合荧光相关光谱和红外吸收光谱,将脂质横向扩散和膜相结构表征为蛋白质与膜表面结合的函数。在支撑膜构型中,霍乱毒素与膜结合的GM1脂质的五糖头基团结合,改变了荧光标记的探针脂质的长程横向扩散,而这些探针脂质不参与结合相互作用。在大多数脂质成分的凝胶-流体转变温度Tm附近,这种效应显著增强。在接近Tm的温度下,在低至0.02面积分数的平均蛋白质覆盖密度下,就可以测量到探针脂质扩散的巨大变化。脂质酰基链中亚甲基对称和不对称伸缩模式的光谱位移证实,蛋白质结合改变了凝胶相中脂质的比例。

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