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2H NMR 证据表明抗生素可诱导生物模型膜中的胆固醇固定化。

2H NMR evidence for antibiotic-induced cholesterol immobilization in biological model membranes.

作者信息

Dufourc E J, Smith I C

出版信息

Biochemistry. 1985 May 7;24(10):2420-4. doi: 10.1021/bi00331a005.

DOI:10.1021/bi00331a005
PMID:4016066
Abstract

The interaction of the polyene antibiotic filipin with membrane sterols has been studied by deuterium nuclear magnetic resonance of the molecular probes [2,2,3,4,4,6-2H6]cholesterol and 1-myristoyl-2-[4',4',14',14',14'-2H5]myristoyl-sn-glycero-3-phospho- choline. At physiological temperatures, there is evidence of filipin-induced cholesterol immobilization in the membrane. The 2H NMR spectra of cholesterol show two domains in which ordering and dynamics are very different. In one of these, cholesterol is static on the 2H NMR time scale, whereas in the other it undergoes rapid axially symmetric motions similar to those it exhibits in the drug-free membrane; this indicates that the jumping frequency of cholesterol between the labile and immobilized domains is less than 10(5) s-1. The distribution of cholesterol between these two sites is temperature dependent; at 0 degrees C all sterol molecules are immobilized, whereas at 60 degrees C they are almost totally in the labile site. In contrast to cholesterol, the phospholipids sense only one type of environment, at both the top and center of the bilayer, indicating that cholesterol acts as a screen, preventing the lipids from direct interaction with the antibiotic. At low temperature, the ordering of the lipid in the presence of cholesterol does not change upon filipin addition, whereas at elevated temperatures the local ordering of both the lipid and the labile cholesterol is significantly lower than that in the absence of the drug. Moreover, there is a very important difference between the degree of local ordering as measured by the lipids and by cholesterol at high temperatures.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

已通过分子探针[2,2,3,4,4,6-2H6]胆固醇和1-肉豆蔻酰基-2-[4',4',14',14',14'-2H5]肉豆蔻酰基-sn-甘油-3-磷酸胆碱的氘核磁共振研究了多烯抗生素制霉菌素与膜甾醇的相互作用。在生理温度下,有证据表明制霉菌素可诱导膜中胆固醇固定。胆固醇的2H NMR光谱显示出两个区域,其有序性和动力学差异很大。在其中一个区域中,胆固醇在2H NMR时间尺度上是静态的,而在另一个区域中,它经历类似于在无药物膜中表现出的快速轴向对称运动;这表明胆固醇在不稳定和固定区域之间的跳跃频率小于10(5) s-1。这两个位点之间胆固醇的分布取决于温度;在0摄氏度时,所有甾醇分子都被固定,而在60摄氏度时,它们几乎完全处于不稳定位点。与胆固醇相反,磷脂在双层的顶部和中心都只感知一种环境,这表明胆固醇起到了屏障作用,防止脂质与抗生素直接相互作用。在低温下,添加制霉菌素后,存在胆固醇时脂质的有序性不变,而在高温下,脂质和不稳定胆固醇的局部有序性均明显低于无药物时。此外,在高温下,通过脂质和胆固醇测量的局部有序度之间存在非常重要的差异。(摘要截短于250字)

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