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阴离子磷脂调节蛋白激酶C过程中脂质双分子层的化学特异性和物理性质:缺乏磷脂酰丝氨酸特异性结合位点的证据

Chemical specificity and physical properties of the lipid bilayer in the regulation of protein kinase C by anionic phospholipids: evidence for the lack of a specific binding site for phosphatidylserine.

作者信息

Mosior M, Golini E S, Epand R M

机构信息

Department of Biochemistry, McMaster University, Hamilton, ON, Canada.

出版信息

Proc Natl Acad Sci U S A. 1996 Mar 5;93(5):1907-12. doi: 10.1073/pnas.93.5.1907.

Abstract

The association of protein kinase C (PKC) with membranes was found not to be specific for phosphatidyl-L-serine (PS). In particular, a synthetic phospholipid, dansyl-phosphatidylethanolamine, proved to be fully functional in the association of PKC with lipid bilayers and in mediating the interaction of this enzyme with diacylglycerol. Dansyl-phosphatidylethanolamine was also able to activate the enzyme in a Ca2+-dependent fashion. Differences in the ability to bind and activate PKC observed for an array of anionic lipids were not larger than alterations caused by changes in acyl chain composition. Thus, although different lipids interact to different extents with PKC, there are no specific binding sites for the PS headgroup on the enzyme. We found that lipids with a greater tendency to form inverted phases increased the binding of PKC to bilayers. However, these changes in lipid structure cannot be considered separately from the miscibility of lipid components in the membrane. For pairs of lipids with similar acyl chains, the dependence on PS concentration is sigmoidal, while for dissimilar acyl chains there is much less dependence of binding on PS concentration. The results can be explained in terms of differences in the lateral distribution of components in the membrane.

摘要

蛋白激酶C(PKC)与膜的结合并非对磷脂酰-L-丝氨酸(PS)具有特异性。特别是,一种合成磷脂,丹磺酰磷脂酰乙醇胺,在PKC与脂质双层的结合以及介导该酶与二酰基甘油的相互作用方面被证明具有完全功能。丹磺酰磷脂酰乙醇胺还能够以Ca2+依赖的方式激活该酶。观察到的一系列阴离子脂质在结合和激活PKC能力上的差异并不比酰基链组成变化引起的改变更大。因此,尽管不同的脂质与PKC的相互作用程度不同,但该酶上不存在PS头部基团的特异性结合位点。我们发现,具有更大倾向形成反相的脂质增加了PKC与双层膜的结合。然而,脂质结构的这些变化不能与膜中脂质成分的混溶性分开考虑。对于具有相似酰基链的脂质对,对PS浓度的依赖性呈S形,而对于不同的酰基链,结合对PS浓度的依赖性要小得多。这些结果可以根据膜中成分横向分布的差异来解释。

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