用ESR光谱比较乙醇和其他抑制剂对大鼠突触体膜序的影响。

Alcohol and drug research Pub Date : 1987-01-01
B J Logan, R Laverty
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引用次数: 0

摘要

采用3种自旋标记探针,比较了乙醇、丁醇和戊巴比酮对大鼠突触体膜的膜顺序的影响,5-羟基硬脂酸从膜表面附近的脂质位点报告,16-羟基硬脂酸从更深的脂质位点报告,马来酰亚胺- tempo与膜蛋白共价结合。降低蛋白结合探针的浓度可提高膜蛋白对乙醇流化效应的敏感性。在乙醇和丁醇麻醉浓度下,三种探针的膜有序度显著降低;戊巴比酮也产生类似的效果,但只有在非常高的浓度下。戊巴比酮在麻醉浓度下引起16-羟基硬脂酸光谱高场峰形状的显著变化;对丁醇和三氯乙醇有轻微的影响,但对乙醇没有影响。这些研究表明,乙醇和戊巴比酮的膜作用位点在ESR探针上是不同的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Comparative effects of ethanol and other depressant drugs on membrane order in rat synaptosomes using ESR spectroscopy.

The effects of ethanol, t-butanol and pentobarbitone on the membrane order of rat synaptosomal membranes have been compared using 3 spin-label probes, 5-doxyl-stearic acid which reports from a lipid site near the membrane surface, 16-doxyl-stearic acid which reports from a deeper lipid site, and maleimide-TEMPO which covalently binds to membrane protein. The sensitivity of the membrane proteins to a fluidizing effect of ethanol was increased by lowering the concentration of protein-binding probe. Significant decreases in membrane order were observed at anaesthetic concentrations of ethanol and t-butanol with all three probes; pentobarbitone produced a similar effect but only at very high concentrations. Pentobarbitone caused a marked change in high-field peak shape of the 16-doxyl-stearic acid spectra at anaesthetic concentrations; this effect was seen slightly with t-butanol and trichlorethanol but not with ethanol. These studies indicate that the membrane sites of action of ethanol and pentobarbitone as shown by ESR probes are different.

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