Effects of Phenylalanine on the Liquid-Expanded and Liquid-Condensed States of Phosphatidylcholine Monolayers.

Lipid insights Pub Date : 2019-01-05 eCollection Date: 2019-01-01 DOI:10.1177/1178635318820923
Andrea C Cutro, E Anibal Disalvo, María A Frías
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引用次数: 4

Abstract

Background: Phenylalanine (Phe) is involved in physiological and pathological processes in cell membranes in which expanded and condensed states coexist. In this direction, it was reported that surface hydration is important for the binding affinity of the amino acid which significantly perturbs 1,2-dipalmitoyl-sn-glycero-3-phosphocholine (DPPC) monolayer structure and morphology. A deeper insight showed that Phe inserts in DPPC monolayer defects as a monomer at pH 5 and forms aggregates that adsorb to the membrane surface generating a reconfiguration of the lipid arrangement in areas of higher packing. This new arrangement in the monolayer causes the reorientation of dipoles of lipid and water molecules which is congruent with the dehydration and surface tension changes reported above. With this background, this article studies the affinity of Phe in liquid-expanded 1,2-dimyristoyl-sn-glycero-3 phosphocholine (LE DMPC) and liquid-condensed 1,2-dipalmitoyl-sn-glycero-3-phosphocholine (LC DPPC) monolayers and their effects on membrane properties.

Results: The adsorption of Phe can be described by a cooperative process in non-independent sites suggesting that Phe/lipid systems reorganize to form new structures at a high degree of coverage. Compressibility modulus and Brewster angle microscopy (BAM) images allow to propose that Phe causes a new phase in 1,2-dimyristoyl-sn-glycero-3 phosphocholine (DMPC) and DPPC.

Conclusions: Phe imposes new arrangements in the lipid phase to form new structures with different compressibility behavior than lipid binary mixtures of DMPC and DPPC. Phe interaction with the LC and LE phases gives place to a process in which a synergistic effect between non-independent sites can be produced. These features of Phe/lipid interaction would be of great importance to understand the multiple effects of Phe on cell membranes.

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苯丙氨酸对磷脂酰胆碱单分子膜液-膨胀和液-凝聚状态的影响。
背景:苯丙氨酸(Phe)参与细胞膜的生理和病理过程,其中扩张和凝聚状态并存。在这个方向上,据报道,表面水合作用对氨基酸的结合亲和力很重要,它显著地扰乱了1,2-双棕榈酰- n-甘油-3-磷脂胆碱(DPPC)单层结构和形态。一项更深入的研究表明,Phe在pH为5时作为单体插入DPPC单层缺陷,并形成聚集体,吸附在膜表面,在更高填料的区域产生脂质排列的重新配置。单分子层中的这种新排列引起脂质和水分子偶极子的重定向,这与上面报道的脱水和表面张力变化是一致的。在此背景下,本文研究了Phe在液体膨胀的1,2-二肉豆醇- n-甘油-3磷酸胆碱(LE DMPC)和液体凝聚的1,2-二棕榈酰- n-甘油-3-磷酸胆碱(LC DPPC)单层膜中的亲和力及其对膜性能的影响。结果:Phe的吸附可以用非独立位点的合作过程来描述,这表明Phe/脂质系统在高度覆盖的情况下重组形成新的结构。压缩模量和Brewster角度显微镜(BAM)图像表明,Phe在1,2-二myristoyl- son -glycero-3 phosphocholine (DMPC)和DPPC中形成了一个新的相。结论:与DMPC和DPPC的脂质二元混合物相比,Phe在脂相中施加新的排列形成新的结构,具有不同的压缩行为。Phe与LC和LE相的相互作用让位于一个过程,在这个过程中,非独立位点之间可以产生协同效应。Phe/脂质相互作用的这些特征对于了解Phe对细胞膜的多重作用具有重要意义。
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