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一种用于紫杉醇水相增溶的新型亲水性嵌段共聚物胶束系统。

A new hydrotropic block copolymer micelle system for aqueous solubilization of paclitaxel.

作者信息

Huh Kang Moo, Min Hyun Su, Lee Sang Cheon, Lee Hong Jae, Kim Sungwon, Park Kinam

机构信息

Department of Polymer Science and Engineering, Chungnam National University, Daejeon 305-764, South Korea.

出版信息

J Control Release. 2008 Mar 3;126(2):122-9. doi: 10.1016/j.jconrel.2007.11.008. Epub 2007 Nov 22.

Abstract

Paclitaxel (PTX), a potent anti-cancer drug, is poorly soluble in water, and this has been a major limitation in developing patient friendly formulations for clinical applications. Recent studies on polymeric micelles, especially hydrotropic polymer micelles, have suggested an alternative formulation of PTX based on their high loading capacity and physical stability in aqueous media. The present study aims at aqueous solubilization of PTX in polymer micelles without using any organic solvents that is usually required for solubilization in polymer micelles. Poly(ethylene glycol) was used as a hydrophilic block and, as a hydrotropic block, poly(4-(2-vinylbenzyloxy-N-picolylnicotinamide)) (P(2-VBOPNA)) was synthesized by atom transfer radical polymerization. The hydrotropic block copolymers did not form a micellar structure at pH 2 or below due to protonation of PNA groups, but the aqueous solubility of PTX increased significantly by the hydrotropic activity of P(2-VBOPNA). At pH values higher than 2, the PTX solubility increased even further due to deprotonation of 2-VBOPNA, leading to effective polymer micellization. A longer hydrotropic block resulted in higher aqueous PTX solubility, and slightly slower release rate from the micelles. The hydrotropic block copolymers synthesized in this study are able to form PTX-loaded polymeric micelles in aqueous solution without using any organic solvents.

摘要

紫杉醇(PTX)是一种强效抗癌药物,在水中溶解度很差,这一直是开发适用于临床应用的患者友好型制剂的主要限制因素。最近对聚合物胶束,特别是水溶助长性聚合物胶束的研究表明,基于其高载药量和在水性介质中的物理稳定性,PTX有另一种制剂形式。本研究旨在不使用聚合物胶束增溶通常所需的任何有机溶剂的情况下,将PTX增溶在聚合物胶束中。聚乙二醇用作亲水嵌段,作为水溶助长嵌段,通过原子转移自由基聚合合成了聚(4-(2-乙烯基苄氧基-N-吡啶甲酰烟酰胺))(P(2-VBOPNA))。由于PNA基团的质子化,水溶助长性嵌段共聚物在pH 2或更低时不会形成胶束结构,但P(2-VBOPNA)的水溶助长活性使PTX的水溶性显著增加。在高于2的pH值下,由于2-VBOPNA的去质子化,PTX的溶解度进一步增加,导致有效的聚合物胶束化。更长的水溶助长嵌段导致更高的PTX水溶性,以及从胶束中释放的速率略慢。本研究中合成的水溶助长性嵌段共聚物能够在不使用任何有机溶剂的情况下,在水溶液中形成负载PTX的聚合物胶束。

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Hydrotropic polymer micelle system for delivery of paclitaxel.用于递送紫杉醇的亲水性聚合物胶束系统
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