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首页> 外文期刊>Journal of cell biology >Effect of streptolysin O on erythrocyte membranes, liposomes, and lipid dispersions. A protein-cholesterol interaction.
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Effect of streptolysin O on erythrocyte membranes, liposomes, and lipid dispersions. A protein-cholesterol interaction.

机译:链球菌溶血素O对红细胞膜,脂质体和脂质分散体的影响。蛋白质-胆固醇相互作用。

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摘要

The effect of the bacterial cytolytic toxin, streptolysin O (SLO), on rabbit erythrocyte membranes, liposomes, and lipid dispersions was examined. SLO produced no gross alterations in the major erythrocyte membrane proteins or lipids. However, when erythrocytes were treated with SLO and examined by electron microscopy, rings and "C"-shaped structures were observed in the cell membrane. The rings had an electron-dense center, 24 nm in diameter, and the overall diameter of the structure was 38 nm. Ring formation also occurred when erythrocyte membranes were fixed with glutaraldehyde and OsO4 before the addition of toxin. In contrast, rings were not seen when erythrocytes were treated with toxin at 0 degrees C, indicating that adsorption of SLO to the membrane is not sufficient for ring formation since toxin is known to bind to erythrocytes at that temperature. The ring structures were present on lecithin-cholesterol-dicetylphosphate liposomes after SLO treatment, but there was no release of the trapped, internal markers, K2CrO4 or glucose. The crucial role of cholesterol in the formation of rings and C's was demonstrated by the fact that these structures were present in toxin-treated cholesterol dispersions, but not in lecithin-dicetylphosphate dispersions nor in the SLO preparations alone. The importance of cholesterol was also shown by the finding that no rings were present in membranes or cholesterol dispersions which had been treated with digitonin before SLO was added. Although rings do not appear to be "holes" in the membrane, a model is proposed which suggests that cholesterol molecules are sequestered during ring and C-structure formation, and that this process plays a role in SLO-induced hemolysis.
机译:检查了细菌溶细胞毒素链球菌溶血素O(SLO)对兔红细胞膜,脂质体和脂质分散体的影响。 SLO在主要的红细胞膜蛋白或脂质中未产生明显变化。然而,当用SLO处理红细胞并通过电子显微镜检查时,在细胞膜中观察到环和“ C”形结构。所述环具有直径为24nm的电子致密中心,并且结构的总直径为38nm。当在添加毒素之前用戊二醛和OsO4固定红细胞膜时也会发生环形成。相反,当在0摄氏度用毒素处理红细胞时,未见到环,这表明SLO在膜上的吸附不足以形成环,因为已知毒素在该温度下会与红细胞结合。 SLO处理后,卵磷脂-胆固醇-二鲸蜡基磷酸酯脂质体上存在环结构,但没有释放出被捕获的内部标记物K2CrO4或葡萄糖。这些结构存在于毒素处理过的胆固醇分散液中,而不存在于卵磷脂-二鲸蜡基磷酸酯分散液中或仅在SLO制剂中,这些事实证明了胆固醇在环和C形成中的关键作用。胆固醇的重要性还通过发现在加入SLO之前用洋地黄皂苷处理过的膜或胆固醇分散液中不存在环的发现得到证明。尽管环似乎不是膜上的“孔”,但提出了一个模型,该模型表明胆固醇分子在环和C结构形成期间被隔离,并且该过程在SLO诱导的溶血中起作用。

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