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首页> 外文期刊>Synthetic and Systems Biotechnology >A high stable pH-temperature dual-sensitive liposome for tuning anticancer drug release
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A high stable pH-temperature dual-sensitive liposome for tuning anticancer drug release

机译:高稳定的pH - 温度双敏脂质体,用于调整抗癌药物释放

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摘要

In order to improve the targeting and availability of liposomes to cancer cells, the temperature sensitivity of 1, 2-Dipalmitoyl-sn-glycero-3-phosphocholine (DPPC) and the pH sensitivity of PASP in PASP-g-C8 are incorporated in a drug delivery system. A composite pH-temperature dual-sensitive liposomes (CPTLPs) was obtained as an efficient drug delivery system. The bionic bilayer is self-assembled by cholesterol/cationic temperature-sensitive lipids as base layer and pH-sensitive octylamine grafted poly aspartic acid (PASP-g-C8) as anchors coated outside. Cytarabine (CYT) was chosen as a model drug. SEM and DLS were used to observe the morphology characteristics of CPTLPs in different micro environment. The results demonstrated that the CPTLPs remained active in both normal (pH7.4 and 37?°C) and tumor tissues (pH 5.0 and 42?°C). As a stable colloidal system, the zeta potential of CPTSLs was ?41.6?mV. In vitro drug-release experiments, the CTY encapsulated dual-sensitive liposomes, CPTSLs(+), not only have significant pH-temperature sensitivity but have more prolonged release in vitro than control groups. MTT tests results indicated that the cell apoptotic effects induced by CPTSLs(+) were nearly 30% higher than the naked drug CTY in HepG2 cells, and 20% lower apoptotic in vero cells. The CPTSLs(+) sustained a stable emulsion form, less toxic effects on normal cells, and exhibited a good pH-temperature sensitivity, thus expected to be a promising tumor targeting drug delivery.
机译:为了改善脂质体对癌细胞的靶向和可用性,将PASP-G-C8的PASP的温度敏感性为1,2-二普利-Sn-甘油-3-普华啉(DPPC)和PHAP-C8的pH敏感性掺入a中药物递送系统。获得复合pH-温度双敏感脂质体(CPTLPS)作为有效的药物递送系统。仿生双层通过胆固醇/阳离子温度敏感的脂质作为基层和pH敏感的辛酸曲胺接枝聚天然酸(PASP-G-C8)作为涂覆的胆固醇/阳离子温度敏感的脂质。选择溶细胞(Cyt)作为模型药物。 SEM和DLS用于观察不同微环境中CPTLP的形态特征。结果表明,CPTLPS在正常(pH7.4和37℃)和肿瘤组织(pH 5.0和42℃)中保持活性。作为稳定的胶体系统,CPTSL的Zeta电位是α41.6?mV。体外药物释放实验,CTY包封的双敏感脂质体,CPTSL(+),不仅具有显着的pH温度敏感性,而且具有比对照组更长的释放。 MTT试验结果表明,CPTSLS(+)诱导的细胞凋亡效应比HepG2细胞中的裸药细胞高于高30%,并且在Vero细胞中凋亡凋亡20%。 CPTSLS(+)持续稳定的乳液形式,对正常细胞的毒性作用较小,并表现出良好的pH温度敏感性,因此预期是靶向药物递送的有前途的肿瘤。

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