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Flower-like curcumin-loaded folic acid-conjugated ZnO-MPA- βcyclodextrin nanostructures enhanced anticancer activity and cellular uptake of curcumin in breast cancer cells

机译:花样的姜黄素加载的叶酸 - 缀合的ZnO-MPa-βcyclodextrin纳米结构增强了抗癌活性和姜黄素的细胞吸收乳腺癌细胞

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Non-spherical structures are beneficial to advance drug delivery effectiveness compared with common spherical ones, due to increased drug loading capability, improved bonding to a vascular wall, enhanced cellular uptake efficacy and prolonged circulation times. In this study, flower-like Zinc oxide-beta cyclodextrin (beta CD) nanostructures functionalized by 3-mercaptopropionic acid (MPA) as a non-spherical delivery system was successfully synthesized for aqueous delivery of curcumin (CUR) to enhance its targeting, bioavailability, and release profile. Terminal carboxyl functional groups were used for the conjugation of folic acid (FA) with the aim of active targeting to folate overexpressing breast cancer cells. The in vitro experimental study and mathematical modeling of CUR release revealed a sustained release with Fickian diffusion as the major release mechanism. MTT, colony formation and Annexin-V FITC/PI assays showed the superior anticancer effect of the system compared to free CUR against breast cancer cell line MDA-MB-231 by promoting the apoptotic respond with no cytotoxic effect on HEK293 normal cells. The efficacy of targeting strategy with FA moieties was demonstrated using the augmented cellular uptake of the FA-conjugated system on overexpressed folate receptor alpha (FR alpha) cells (MDA-MB-468 breast cancer cell line). Furthermore, loading of CUR to the delivery systems significantly lowered the MIC values (2.5 to 5-fold) against S. aureus and E. coli the infections of which are serious problems in cancer patients. According to the results of this study, the system can serve as a promising non-spherical delivery vehicle for enhancing bioavailability and targeting of hydrophobic anticancer agents in the future.
机译:由于药物负载能力增加,与常见的球形壁增加,与血管壁增加,增强蜂窝摄取功效和延长循环时间,有利于预先推进药物递送效率的有益的药物递送效果。在该研究中,成功​​地合成了由3-巯基丙酸(MPa)作为非球形递送系统官能化的花样的氧化锌 - β-β-β-β(β)纳米结构,用于含水递送姜黄素(Cur),以增强其靶向,生物利用度和释放概况。末端羧基官能团用于叶酸(FA)的缀合,目的是活性靶向叶酸过度表达乳腺癌细胞。 Cur释放的体外实验研究和数学建模显示了Fickian扩散作为主要释放机制的持续释放。 MTT,菌落形成和Annexin-V FITC / PI测定显示系统的优异抗癌效果与乳腺癌细胞系MDA-MB-231相比,通过促进细胞毒性作用对HEK293正常细胞没有细胞毒性作用。使用FA缀合系统对过表达叶酸受体α(FRα)细胞(MDA-MB-468乳腺癌细胞系)的增强细胞吸收来证明靶向策略与FA部分的疗效。此外,加载到输送系统的CUR的加载显着降低了对金黄色葡萄球菌的MIC值(2.5至5倍),并且大肠杆菌是癌症患者的严重问题。根据该研究的结果,该系统可以作为未来增强生物利用度和疏水抗癌剂的生物利用度和靶向的有前途的非球形递送载体。

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