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首页> 外文期刊>RSC Advances >Liposome collapse resulting from an allosteric interaction between 2,6-dimethyl-β-cyclodextrins and lipids
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Liposome collapse resulting from an allosteric interaction between 2,6-dimethyl-β-cyclodextrins and lipids

机译:脂质体塌陷由2,6-二甲基-β-环糊精和脂质之间的变形相互作用产生

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摘要

Although heptakis(2,6-di- O -methyl)-β-cyclodextrin (DMe-β-CDx) has been reported to exhibit higher cytotoxicity than many other cyclodextrins because of the way in which it abstracts cholesterols from liposomes, we have identified another reason for its cytotoxicity based on its interaction with lipids. These interactions exhibited nonlinear sigmoidal responses with Hill coefficient values ( n ) in the range of 3.0–3.6, which indicated that this phenomenon involves positive allosterism. Furthermore, analysis by mass spectroscopy revealed that the lipid–DMe-β-CDx complexes had stoichiometric ratios in the range of 1?:?1–1?:?4.
机译:据报道,七(2,6-二甲基)-β-环糊精(DME-β-CDX)表现出比许多其他环糊精的细胞毒性更高,因为它鉴定了脂质体的胆固醇的方式,但我们已经确定了基于其与脂质相互作用的细胞毒性的另一个原因。这些相互作用在3.0-3.6的范围内表现出与山脉系数值(n)的非线性六样响应,这表明这种现象涉及积极的颠振。此外,通过质谱分析显示,脂质-DME-β-CDX复合物在1的范围内具有化学计量比率,在1?:1-1?:?4。

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