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用差示扫描量热法研究甾醇-尿苷缀合物与 DMPC 脂质体的相互作用。

Synthesis and interaction of sterol-uridine conjugate with DMPC liposomes studied by differential scanning calorimetry.

机构信息

Grupo Productos Naturales Marinos, Facultad de Ciencias Farmacéuticas y Alimentarias, Universidad de Antioquia, UdeA, Calle 70 No 52-21, Medellín, Colombia.

Grupo Productos Naturales Marinos, Facultad de Ciencias Farmacéuticas y Alimentarias, Universidad de Antioquia, UdeA, Calle 70 No 52-21, Medellín, Colombia; Instituto de Física, Universidad de Antioquia, UdeA, Calle 70 No 52-21, Medellín, Colombia.

出版信息

Colloids Surf B Biointerfaces. 2018 Jun 1;166:203-209. doi: 10.1016/j.colsurfb.2018.03.023. Epub 2018 Mar 19.

DOI:10.1016/j.colsurfb.2018.03.023
PMID:29597153
Abstract

Differential scanning calorimetry (DSC) is a thermoanalytical technique which provides information on the interaction between drugs and models of cell membranes. Studies on the calorimetric behavior of hydrated phospholipids within liposomes are employed to shed light on the changes in the physico-chemical properties when interacting with drugs. In this report, new potential anti-cancer drugs such as uridine and uridine derivatives (acetonide and its succinate), 3β-5α,8α-endoperoxide-cholestan-6-en-3-ol (5,8-epidioxicholesterol) and conjugate (uridine acetonide-epidioxicholesterol succinate) have been synthesized. Steglich esterification method using coupling agents allowed to obtain the uridine acetonide-sterol conjugate. The study on the interaction between the drugs and dimiristoyl-phophatidilcholine (DMPC) liposomes has been conducted by the use of DSC. The analysis of the DSC curves indicated that the uridine and derivatives (acetonide and its succinate) present a very soft interaction with the DMPC liposomes, whereas the 5,8-epidioxicholesterol and the conjugate showed a strong effect on the thermotropic behavior. Our results suggested that the lipophilic character of uridine acetonide-sterol conjugate improves the affinity with the DMPC liposomes.

摘要

差示扫描量热法(DSC)是一种热分析技术,可提供药物与细胞膜模型相互作用的信息。研究水合磷脂在脂质体中的量热行为有助于了解与药物相互作用时物理化学性质的变化。在本报告中,已经合成了新的潜在抗癌药物,如尿苷和尿苷衍生物(乙酰亚胺和琥珀酸酯)、3β-5α,8α-内过氧化物-胆甾烷-6-烯-3-醇(5,8-表二氧胆固醇)和共轭物(尿苷乙酰亚胺-表二氧胆固醇琥珀酸酯)。使用偶联剂Steglich 酯化法可以获得尿苷乙酰亚胺-甾醇共轭物。通过 DSC 研究了药物与二肉豆蔻酰磷脂酰胆碱(DMPC)脂质体之间的相互作用。DSC 曲线的分析表明,尿苷及其衍生物(乙酰亚胺和琥珀酸酯)与 DMPC 脂质体之间存在非常软的相互作用,而 5,8-表二氧胆固醇及其共轭物对热致行为有强烈影响。我们的结果表明,尿苷乙酰亚胺-甾醇共轭物的亲脂性提高了与 DMPC 脂质体的亲和力。

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