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肌动蛋白与膜脂之间的相互作用机制:压力调谐红外光谱研究

Mechanism of interaction between actin and membrane lipids: a pressure-tuning infrared spectroscopy study.

作者信息

Gicquaud C, Wong P

机构信息

Département de Chimie Biologie, Université de Québec à Trois Rivières, Canada.

出版信息

Biochem J. 1994 Nov 1;303 ( Pt 3)(Pt 3):769-74. doi: 10.1042/bj3030769.

Abstract

Using pressure-tuning Fourier transform infrared spectroscopy to study an in vitro system consisting of actin and distearoyl-phosphatidylcholine (DSPC) liposomes, we have determined the mechanism of interaction between actin and membrane lipids. This interaction results in a significant conformational change in actin molecules. Analysis of the amide I band of actin shows an increase in the beta-sheets to alpha-helix ratio, in random turns, and in interactions between actin monomers. In the absence of lipids, the actin molecules are denatured by pressures of 8 x 10(8) Pa and more, which give rise to a random organization of the peptide chain. However, in the presence of DSPC liposomes, pressure greater than 2 x 10(8) Pa induces a change in actin conformation, which is dominated by strongly interacting beta-sheets. As the spectra of the lipid molecules are not changed by the presence of actin, the organization of the lipid molecules in the bilayer is not affected by the protein. It is concluded from these results that this interaction of actin with membrane lipids involves very few lipid molecules. These lipid molecules may interact with actin at a few specific sites on the protein.

摘要

利用压力调谐傅里叶变换红外光谱研究由肌动蛋白和二硬脂酰磷脂酰胆碱(DSPC)脂质体组成的体外系统,我们确定了肌动蛋白与膜脂之间的相互作用机制。这种相互作用导致肌动蛋白分子发生显著的构象变化。对肌动蛋白酰胺I带的分析表明,β-折叠与α-螺旋的比例、无规卷曲以及肌动蛋白单体之间的相互作用均有所增加。在没有脂质的情况下,肌动蛋白分子在8×10⁸ Pa及更高的压力下会变性,导致肽链呈现无规排列。然而,在存在DSPC脂质体的情况下,大于2×10⁸ Pa的压力会诱导肌动蛋白构象发生变化,这种变化以强烈相互作用的β-折叠为主导。由于肌动蛋白的存在并未改变脂质分子的光谱,因此双层脂质分子的排列不受蛋白质的影响。从这些结果可以得出结论,肌动蛋白与膜脂的这种相互作用只涉及极少数脂质分子。这些脂质分子可能在蛋白质上的几个特定位点与肌动蛋白相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99af/1137613/334e48a29f7b/biochemj00076-0094-a.jpg

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