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[冰片与叶酸共修饰载阿霉素PAMAM药物递送系统的制备及体外评价]

[Preparation and in vitro evaluation of borneol and folic acid co-modified doxorubicin loaded PAMAM drug delivery system].

作者信息

Li Jing-jing, Guo Man-man, Han Shun-ping, Sun Yue, Fei Wei-dong, Xu Xiu-iing, Li Fan-zhu

出版信息

Yao Xue Xue Bao. 2015 Jul;50(7):899-905.

Abstract

A novel targeting drug carrier (FA-BO-PAMAM) based on the PAMAM G5 dendrimer modified with borneol (BO) and folic acid (FA) molecules on the periphery and doxorubicin (DOX) loaded in the interior was designed and prepared to achieve the purposes of enhancing the blood-brain barrier (BBB) transportation and improving the drug accumulation in the glioma cells. 1H NMR was used to confirm the synthesis of FA-BO-PAMAM; its morphology and mean size were analyzed by dynamic light scattering (DLS) and transmission electron microscope (TEM). Based on the HBMEC and C6 cells, cytotoxicity assay, transport across the BBB, cellular uptake and anti-tumor activity in vitro were investigated to evaluate the properties of nanocarriers in vitro. The results showed that the nanocarrier of FA-BO-PAMAM was successfully synthesized, which was spherical in morphology with the average size of (22.28 ± 0.42) nm, and zeta potential of (7.6 ± 0.89) mV. Cytotoxicity and transport across the BBB assay showed that BO-modified conjugates decreased the cytotoxicity of PAMAM against both HBMEC and C6 cells and exhibited higher BBB transportation ability than BO-unmodified conjugates; moreover, modification with FA increased the total uptake of DOX by C6 cells and enhanced the cytotoxicity of DOX-polymer against C6 cells. Therefore, FA-BO-PAMAM is a promising nanodrug delivery system in employing PAMAM as a drug carrier and treatment for brain glioma.

摘要

设计并制备了一种新型靶向药物载体(FA-BO-PAMAM),其基于在外围用冰片(BO)和叶酸(FA)分子修饰的聚酰胺-胺(PAMAM)G5树枝状大分子,并在内部负载阿霉素(DOX),以实现增强血脑屏障(BBB)转运和提高胶质瘤细胞中药物蓄积的目的。利用1H NMR确认FA-BO-PAMAM的合成;通过动态光散射(DLS)和透射电子显微镜(TEM)分析其形态和平均尺寸。基于人脑微血管内皮细胞(HBMEC)和C6细胞,研究了细胞毒性测定、BBB转运、细胞摄取和体外抗肿瘤活性,以评估纳米载体的体外性质。结果表明,成功合成了FA-BO-PAMAM纳米载体,其形态为球形,平均尺寸为(22.28±0.42)nm,zeta电位为(7.6±0.89)mV。细胞毒性和BBB转运测定表明,BO修饰的缀合物降低了PAMAM对HBMEC和C6细胞的细胞毒性,并且比未修饰BO的缀合物表现出更高的BBB转运能力;此外,用FA修饰增加了C6细胞对DOX的总摄取,并增强了DOX-聚合物对C6细胞的细胞毒性。因此,FA-BO-PAMAM作为一种以PAMAM为药物载体治疗脑胶质瘤的纳米药物递送系统具有广阔前景。

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