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芘标记的磷酸脂和鞘脂在有序和无序双层结构域之间的分配。

Partitioning of pyrene-labeled phospho- and sphingolipids between ordered and disordered bilayer domains.

作者信息

Koivusalo Mirkka, Alvesalo Joni, Virtanen Jorma A, Somerharju Pentti

机构信息

Institute of Biomedicine, Department of Biochemistry, University of Helsinki, Helsinki, Finland.

出版信息

Biophys J. 2004 Feb;86(2):923-35. doi: 10.1016/S0006-3495(04)74168-5.

Abstract

Here we have studied how the length of the pyrene-labeled acyl chain (n) of a phosphatidylcholine, sphingomyelin, or galactosylceramide affects the partitioning of these lipids between 1), gel and fluid domains coexisting in bovine brain sphingomyelin (BB-SM) or BB-SM/spin-labeled phosphatidylcholine (PC) bilayers or 2), between liquid-disordered and liquid-ordered domains in BB-SM/spin-labeled PC/cholesterol bilayers. The partitioning behavior was deduced either from modeling of pyrene excimer/monomer ratio versus temperature plots, or from quenching of the pyrene monomer fluorescence by spin-labeled PC. New methods were developed to model excimer formation and pyrene lipid quenching in segregated bilayers. The main result is that partition to either gel or liquid-ordered domains increased significantly with increasing length of the labeled acyl chain, probably because the pyrene moiety attached to a long chain perturbs these ordered domains less. Differences in partitioning were also observed between phosphatidylcholine, sphingomyelin, and galactosylceramide, thus indicating that the lipid backbone and headgroup-specific properties are not severely masked by the pyrene moiety. We conclude that pyrene-labeled lipids could be valuable tools when monitoring domain formation in model and biological membranes as well as when assessing the role of membrane domains in lipid trafficking and sorting.

摘要

在此,我们研究了磷脂酰胆碱、鞘磷脂或半乳糖神经酰胺的芘标记酰基链长度(n)如何影响这些脂质在以下两种情况之间的分配:1)在牛脑鞘磷脂(BB-SM)或BB-SM/自旋标记磷脂酰胆碱(PC)双层中共存的凝胶态和流体态区域之间;2)在BB-SM/自旋标记PC/胆固醇双层中的液相无序和液相有序区域之间。分配行为可通过芘激基缔合物/单体比率对温度的曲线建模推导得出,也可通过自旋标记PC对芘单体荧光的猝灭推导得出。我们开发了新方法来模拟隔离双层中激基缔合物的形成和芘脂质猝灭。主要结果是,随着标记酰基链长度的增加,分配到凝胶态或液相有序区域的比例显著增加,这可能是因为连接到长链上的芘部分对这些有序区域的扰动较小。在磷脂酰胆碱、鞘磷脂和半乳糖神经酰胺之间也观察到了分配差异,因此表明脂质主链和头基特异性性质并未被芘部分严重掩盖。我们得出结论,芘标记的脂质在监测模型膜和生物膜中的区域形成以及评估膜区域在脂质运输和分选中的作用时可能是有价值的工具。

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