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首页> 外文期刊>ACS Omega >Amphiphilic Small-Molecule Assemblies to Enhance the Solubility and Stability of Hydrophobic Drugs
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Amphiphilic Small-Molecule Assemblies to Enhance the Solubility and Stability of Hydrophobic Drugs

机译:两亲的小分子组件,增强疏水性药物的溶解度和稳定性

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Amphiphilic assemblies made from diverse synthetic building blocks are well known for their biomedical applications. Here, we report the synthesis of gemini-type amphiphilic molecules that form stable assemblies in water. The assembly property of molecule M2 in aqueous solutions was first inferred from peak broadening observed in the proton NMR spectrum. This was supported by dynamic light scattering and transmission electron microscopy analysis. The assembly formed from M2 (M2_(agg)) was used to solubilize the hydrophobic drugs curcumin and doxorubicin at physiological pH. M2_(agg) was able to effectively solubilize curcumin as well as protect it from degradation under UV irradiation. Upon solubilization in M2_(agg), curcumin showed excellent cell permeability and higher toxicity to cancer cells over normal cells, probably because of enhanced cellular uptake and increased stability. M2_(agg) also showed pH-dependent release of doxorubicin, resulting in controlled toxicity on cancer cell lines, making it a promising candidate for the selective delivery of drugs to cancer cells.
机译:由各种合成构建块制成的两亲性装配是其生物医学应用众所周知的。在这里,我们报告了在水中形成稳定组件的双子型两亲分子的合成。首先从质子NMR光谱中观察到水溶液中分子M2在水溶液中的组装特性。这是通过动态光散射和透射电子显微镜分析来支持的。由M2形成的组件(M2_(agg))用于在生理pH下溶解疏水药物姜黄素和多柔比星。 M2_(AGG)能够有效地溶解姜黄素,并保护其免受紫外线照射下的降解。在M2_(AGG)中的溶解后,姜黄素显示出优异的细胞渗透性和对癌细胞上常细胞上的癌细胞更高的毒性,可能是因为增强的细胞吸收和增加的稳定性。 M2_(AGG)还显示了多柔比星的pH依赖性释放,导致对癌细胞系的受控毒性,使其成为对癌细胞选择性递送药物的有希望的候选者。

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