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用于被动肿瘤靶向的阿霉素与接枝HPMA共聚物的缀合物。

Conjugates of doxorubicin with graft HPMA copolymers for passive tumor targeting.

作者信息

Etrych Tomás, Chytil Petr, Mrkvan Tomás, Sírová Milada, Ríhová Blanka, Ulbrich Karel

机构信息

Institute of Macromolecular Chemistry AS CR, v.v.i., Heyrovský Sq. 2, 162 06 Prague 6, Czech Republic.

出版信息

J Control Release. 2008 Dec 18;132(3):184-92. doi: 10.1016/j.jconrel.2008.04.017. Epub 2008 Apr 29.

DOI:10.1016/j.jconrel.2008.04.017
PMID:18534705
Abstract

Synthesis, physicochemical behavior, tumor accumulation and preliminary anticancer activity of a new biodegradable graft copolymer-doxorubicin (DOX) conjugates designed for passive tumor targeting were investigated. In the graft high-molecular-weight conjugates the multivalent N-(2-hydroxypropyl)methacrylamide (HPMA) copolymer was grafted with a similar but semitelechelic HPMA copolymer; both types of polymer chains were bearing doxorubicin attached by hydrazone bonds enabling intracellular pH-controlled drug release. The polymer grafts were attached to the main chain through spacers, degradable enzymatically or reductively, facilitating, after the drug release, intracellular degradation of the graft polymer carrier to short fragments excretable from the organism by glomerular filtration. The graft polymer-DOX conjugate exhibited prolonged blood circulation and enhanced tumor accumulation in tumor-bearing mice indicating the important role of the EPR effect in the anticancer activity. The graft polymer-DOX conjugates showed a significantly higher antitumor activity in vivo than DOX.HCl or the linear polymer conjugate when tested in mice bearing 38C13 B-cell or EL4 T-cell lymphoma, with a significant number of long-term-surviving (LTS) mice with EL4 T-cell lymphoma treated with a single dose 15 mg DOX equiv./kg on day 10.

摘要

研究了一种设计用于被动肿瘤靶向的新型可生物降解接枝共聚物-阿霉素(DOX)缀合物的合成、物理化学行为、肿瘤蓄积及初步抗癌活性。在接枝高分子量缀合物中,多价N-(2-羟丙基)甲基丙烯酰胺(HPMA)共聚物与一种类似但半遥爪的HPMA共聚物接枝;两种类型的聚合物链均带有通过腙键连接的阿霉素,实现细胞内pH控制的药物释放。聚合物接枝物通过可酶解或还原降解的间隔基连接到主链上,在药物释放后,促进接枝聚合物载体在细胞内降解为可通过肾小球滤过从体内排出的短片段。接枝聚合物-DOX缀合物在荷瘤小鼠中表现出延长的血液循环和增强的肿瘤蓄积,表明EPR效应在抗癌活性中的重要作用。当在携带38C13 B细胞或EL4 T细胞淋巴瘤的小鼠中进行测试时,接枝聚合物-DOX缀合物在体内显示出比阿霉素盐酸盐或线性聚合物缀合物显著更高的抗肿瘤活性,在第10天用15 mg DOX当量/kg的单剂量治疗的携带EL4 T细胞淋巴瘤的小鼠中有大量长期存活(LTS)小鼠。

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