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Enhanced Solubility and Anticancer Potential of Mansonone G By β-Cyclodextrin-Based Host-Guest Complexation: A Computational and Experimental Study

机译:基于β-环糊精的宿主-客体复合物增强甘露酮G的溶解度和抗癌潜力:计算和实验研究

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摘要

Mansonone G (MG), a plant-derived compound isolated from the heartwood of , possesses a potent antitumor effect on several kinds of malignancy. However, its poor solubility limits the use for practical applications. Beta-cyclodextrin (βCD), a cyclic oligosaccharide composed of seven (1→4)-linked α-D-glucopyranose units, is capable of encapsulating a variety of poorly soluble compounds into its hydrophobic interior. In this work, we aimed to enhance the water solubility and the anticancer activity of MG by complexation with βCD and its derivatives (2,6-di- -methyl-βCD (DMβCD) and hydroxypropyl-βCD). The 90-ns molecular dynamics simulations and MM/GBSA-based binding free energy results suggested that DMβCD was the most preferential host molecule for MG inclusion complexation. The inclusion complex formation between MG and βCD(s) was confirmed by DSC and SEM techniques. Notably, the MG/βCDs inclusion complexes exerted significantly higher cytotoxic effect (~2–7 fold) on A549 lung cancer cells than the uncomplexed MG.
机译:Mansonone G(MG)是一种从植物心材中分离的植物来源化合物,对多种恶性肿瘤具有有效的抗肿瘤作用。然而,其差的溶解度限制了其在实际应用中的用途。 β-环糊精(βCD)是一种由七个(1→4)连接的α-D-吡喃葡萄糖单元组成的环状低聚糖,能够将多种难溶性化合物封装在其疏水内部。在这项工作中,我们旨在通过与βCD及其衍生物(2,6-二-甲基-βCD(DMβCD)和羟丙基-βCD)络合来增强MG的水溶性和抗癌活性。 90 ns的分子动力学模拟和基于MM / GBSA的结合自由能结果表明DMβCD是MG包合物络合的最优先宿主分子。通过DSC和SEM技术证实了MG和βCD之间的包合物形成。值得注意的是,与未复合的MG相比,MG /βCDs包含复合物对A549肺癌细胞的杀伤作用明显更高(约2-7倍)。

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