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溶血脂质与脂质囊泡膜的交换。

Lysolipid exchange with lipid vesicle membranes.

作者信息

Needham D, Zhelev D V

机构信息

Department of Mechanical Engineering and Materials Science, Duck University, Durham, NC, USA.

出版信息

Ann Biomed Eng. 1995 May-Jun;23(3):287-98. doi: 10.1007/BF02584429.

DOI:10.1007/BF02584429
PMID:7631982
Abstract

While the aqueous solubility for bilayer phospholipids is less than 10(-10) M--keeping lipid membranes at essentially constant mass, single chain surfactants can have a significant aqueous solubility. Thus, in surfactant solutions, both monomer and micelles can interact with a lipid bilayer, and the mass and composition of the bilayer can be changed in seconds. These changes in composition are expected to have direct consequences on bilayer structure and material properties. We have found that the exchange of surfactants like lysolecithin can be described in terms of a kinetic model in which monomer and micelles are transported to the membrane from bulk solution. Molecular transport is considered at the membrane interfaces and across the midplane between the two monolayers of the bilayer. Using micropipet manipulation, single vesicles were transferred into lysolecithin solutions, and the measurement of vesicle area change gave a direct measure of lysolecithin uptake. Transfer back to lysolecithin-free media resulted in desorption. The rates of uptake and desorption could therefore be measured at controlled levels of membrane stress. With increasing lysolecithin concentration in the bulk phase, the amount of lysolecithin in the membrane reached saturation at approximately 3 mol% for concentrations below the critical micelle concentration (CMC) and at > 30 mol% for concentrations above the CMC. When convective transport was used to deliver lysolecithin, uptake occurred via a double exponential: initial uptake into the outer monolayer was fast (approximately 0.2 sec-1); transfer across the bilayer midplane was much slower (0.0019 sec-1).

摘要

虽然双层磷脂的水溶性小于10^(-10) M(这使得脂质膜的质量基本保持恒定),但单链表面活性剂却具有显著的水溶性。因此,在表面活性剂溶液中,单体和胶束都能与脂质双层相互作用,并且双层的质量和组成可在数秒内发生变化。这些组成上的变化预计会对双层结构和材料特性产生直接影响。我们发现,像溶血卵磷脂这样的表面活性剂的交换可以用一个动力学模型来描述,在该模型中,单体和胶束从本体溶液被转运到膜上。分子转运在膜界面以及双层两个单分子层之间的中平面进行考虑。使用微量移液管操作,将单个囊泡转移到溶血卵磷脂溶液中,通过测量囊泡面积变化可直接测定溶血卵磷脂的摄取量。再转移回无溶血卵磷脂的介质中会导致解吸。因此,可以在可控的膜应力水平下测量摄取和解吸速率。随着本体相中溶血卵磷脂浓度的增加,对于低于临界胶束浓度(CMC)的浓度,膜中溶血卵磷脂的量在约3 mol%时达到饱和;对于高于CMC的浓度,该量在> 30 mol%时达到饱和。当使用对流运输来递送溶血卵磷脂时,摄取过程呈现双指数形式:最初快速摄取到外层单分子层(约0.2秒^(-1));跨双层中平面的转移则慢得多(0.0019秒^(-1))。

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