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带电麻醉剂通过内膜或外膜小叶的选择性流化作用改变肺成纤维细胞质膜酶。

Charged anaesthetics alter LM-fibroblast plasma-membrane enzymes by selective fluidization of inner or outer membrane leaflets.

作者信息

Sweet W D, Schroeder F

出版信息

Biochem J. 1986 Oct 15;239(2):301-10. doi: 10.1042/bj2390301.

Abstract

The functional consequences of the differences in lipid composition and structure between the two leaflets of the plasma membrane were investigated. Fluorescence of 1,6-diphenylhexa-1,3,5-triene(DPH), quenching, and differential polarized phase fluorimetry demonstrated selective fluidization by local anaesthetics of individual leaflets in isolated LM-cell plasma membranes. As measured by decreased limiting anisotropy of DPH fluorescence, cationic (prilocaine) and anionic (phenobarbital and pentobarbital) amphipaths preferentially fluidized the cytofacial and exofacial leaflets respectively. Unlike prilocaine, procaine, also a cation, fluidized both leaflets of these membranes equally. Pentobarbital stimulated 5'-nucleotidase between 0.1 and 5 mM and inhibited at higher concentrations, whereas phenobarbital only inhibited, at higher concentrations. Cationic drugs were ineffective. Two maxima of (Na+ + K+)-ATPase activation were obtained with both anionic drugs. Only one activation maximum was obtained with both cationic drugs. The maximum in activity below 1 mM for all four drugs clustered about a single limiting anisotropy value in the cytofacial leaflet, whereas there was no correlation between activity and limiting anisotropy in the exofacial leaflets. Therefore, although phenobarbital and pentobarbital below 1 mM fluidized the exofacial leaflet more than the cytofacial leaflet, the smaller fluidization in the cytofacial leaflet was functionally significant for (Na+ + K+)-ATPase. Mg2+-ATPase was stimulated at 1 mM-phenobarbital, unaffected by pentobarbital and slightly stimulated by both cationic drugs at concentrations fluidizing both leaflets. Thus the activity of (Na+ + K+)-ATPase was highly sensitive to selective fluidization of the leaflet containing its active site, whereas the other enzymes examined were little affected by fluidization of either leaflet.

摘要

研究了质膜两个小叶在脂质组成和结构上的差异所产生的功能后果。1,6 - 二苯基己三烯(DPH)荧光、猝灭和差分偏振相荧光测定法表明,局麻药可使分离的LM细胞质膜中单个小叶选择性地发生流化。通过DPH荧光极限各向异性降低来衡量,阳离子型(丙胺卡因)和阴离子型(苯巴比妥和戊巴比妥)两亲物分别优先使细胞质小叶和细胞外小叶发生流化。与丙胺卡因不同,同样是阳离子的普鲁卡因能使这些膜的两个小叶同等程度地流化。戊巴比妥在0.1至5 mM之间刺激5'-核苷酸酶,在较高浓度时则抑制,而苯巴比妥仅在较高浓度时抑制,阳离子药物则无效。两种阴离子药物都获得了(Na + + K +)-ATP酶激活的两个最大值。两种阳离子药物都只获得了一个激活最大值。所有四种药物在低于1 mM时活性的最大值在细胞质小叶中聚集在一个单一的极限各向异性值附近,而在细胞外小叶中活性与极限各向异性之间没有相关性。因此,尽管低于1 mM的苯巴比妥和戊巴比妥使细胞外小叶的流化程度大于细胞质小叶,但细胞质小叶中较小程度的流化对(Na + + K +)-ATP酶在功能上具有重要意义。Mg2 + -ATP酶在1 mM苯巴比妥时受到刺激,不受戊巴比妥影响,并且在使两个小叶都流化的浓度下,两种阳离子药物都对其有轻微刺激。因此,(Na + + K +)-ATP酶的活性对含有其活性位点的小叶的选择性流化高度敏感,而所检测的其他酶受任何一个小叶流化的影响都很小。

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