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基于泊洛沙姆 407 的温敏性胶束-水凝胶杂化系统用于紫杉醇的局部递送。

Thermosensitive micelles-hydrogel hybrid system based on poloxamer 407 for localized delivery of paclitaxel.

机构信息

Center of Drug Discovery, State Key Laboratory of Natural Medicines, China Pharmaceutical University, Nanjing 210009, PR China.

出版信息

J Pharm Sci. 2013 Aug;102(8):2707-17. doi: 10.1002/jps.23649. Epub 2013 Jul 9.

DOI:10.1002/jps.23649
PMID:23839931
Abstract

A thermosensitive micelles-hydrogel hybrid system based on Poloxamer 407 (P407) was prepared to resolve the fast erosion and low loading capability of lipophilic drug of P407 gels for local chemotherapy. Different amounts of glutaraldehyde (GA) were applied to generate cross-linked networks with carboxymethyl chitosan (CMCS) interpenetrated in P407 gels, in which paclitaxel (PTX)-loaded N-octyl-O-sulfate chitosan micelles (PTX-M) were dispersed uniformly. The in vitro characteristics of CMCS-modified P407 gels (PTX-M-MG) were performed by examining the viscosity, swelling ratio, mechanical property, and drug release, while the in vivo evaluation included tissue distribution and anticancer efficacy through intratumoral administration in hepatoma solidity cell (Heps) tumor-bearing mice. The results showed that PTX-M-MG containing 0.05% (w/v) GA possessed lower viscosity, higher swelling ratio, stronger mechanical property, and longer term drug release, in which the loading efficiency of PTX was enlarged by the introduction of PTX-M. Moreover, PTX-M-MG revealed a prolonged retention at tumor sites, lasting for 20 days, and a superior tumor inhibition rate (64.27%) with reduced toxicity compared with Taxol(®) , PTX-M, and PTX-M loaded unmodified P407 gels (PTX-M-P407). It can be concluded that PTX-M-MG is a promising local delivery system for hydrophobic drug in cancer therapy, providing both improved efficacy and relieved side effects.

摘要

一种基于泊洛沙姆 407(P407)的温敏胶束-水凝胶杂化系统被制备用于解决 P407 凝胶作为局部化疗的亲脂性药物的快速侵蚀和低载药量问题。用不同量的戊二醛(GA)与互穿的羧甲基壳聚糖(CMCS)生成交联网络,其中紫杉醇(PTX)负载的辛基-O-磺酸壳聚糖胶束(PTX-M)均匀分散。通过考察粘度、溶胀比、力学性能和药物释放,对 CMCS 修饰的 P407 凝胶(PTX-M-MG)的体外特性进行了研究,体内评价包括通过荷肝癌实体细胞(Heps)肿瘤小鼠瘤内给药进行组织分布和抗癌疗效。结果表明,含 0.05%(w/v)GA 的 PTX-M-MG 具有较低的粘度、较高的溶胀比、较强的力学性能和较长的药物释放时间,其中 PTX-M 的引入增大了 PTX 的载药量。此外,PTX-M-MG 在肿瘤部位的滞留时间延长至 20 天,与 Taxol(®)、PTX-M 和负载未修饰的 P407 凝胶的 PTX-M(PTX-M-P407)相比,具有更好的肿瘤抑制率(64.27%)和较低的毒性。综上所述,PTX-M-MG 是一种有前途的用于癌症治疗的疏水性药物的局部给药系统,既能提高疗效又能减轻副作用。

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