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Carbon nanotube lipid drug approach for targeted delivery of a chemotherapy drug in a human breast cancer xenograft animal model

机译:碳纳米管脂质药物在人类乳腺癌异种移植动物模型中靶向递送化疗药物的方法

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Carbon nanotube (CNT) possesses excellent properties as a drug carrier. To overcome the challenge of drug functionalization with CNT, we have developed a lipid-drug approach for efficient drug loading onto CNT, in which a long chain lipid molecule is conjugated to the drug molecule so that the lipid-drug can be loaded directly onto CNT through binding of the lipid 'tail' in the drug molecule to CNT surfaces via hydrophobic interactions. In a proof-of-concept study, drug paclitaxel (PTX) was conjugated with a non-toxic lipid molecule docosanol for functionalization with CNT. Folic acid was also conjugated to CNT for targeted drug delivery. High level of drug loading onto SWNT could be achieved by lipid-drug approach. Conjugation of FA to SWNT-lipid-PTX led to an increase in cell penetration capacity, and the targeted SWNT-lipid-PTX showed much improved drug efficacy invitro in comparison to free drug Taxol and non-targeted SWNT-lipid-PTX at 48h (78.5% vs. 31.6% and 59.1% in cytotoxicity respectively, p<0.01). Invivo analysis using a human breast cancer xenograft mice model also confirmed the improved drug efficacy. The targeted SWNT-lipid-PTX was found non-toxic as evaluated by biochemical analysis using blood samples, and by histological analysis of major organs.
机译:碳纳米管(CNT)具有出色的药物载体性能。为了克服使用CNT进行药物功能化的挑战,我们开发了一种将有效药物加载到CNT的脂质-药物方法,其中将长链脂质分子与药物分子偶联,以便可以将脂质-药物直接加载到CNT上。通过疏水性相互作用使药物分子中的脂质“尾巴”与CNT表面结合。在概念验证研究中,将紫杉醇(PTX)与无毒脂质分子二十二烷醇偶联以用于CNT官能化。叶酸还与CNT结合以用于靶向药物递送。通过脂质-药物方法可以实现将高水平的药物负载到SWNT上。 FA与SWNT-脂质-PTX的结合导致细胞穿透能力的增加,并且与游离药物紫杉醇和非靶向SWNT-脂质-PTX在48h相比,靶向SWNT-脂质-PTX的体外药物功效大大提高(细胞毒性分别为78.5%和31.6%和59.1%,p <0.01)。使用人乳腺癌异种移植小鼠模型的体内分析也证实了改善的药物疗效。通过使用血样的生化分析和主要器官的组织学分析,发现靶向的SWNT-脂质-PTX无毒。

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