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聚-L-天冬氨酸作为阿霉素载体:游离药物与聚合物结合药物的体内比较研究

Poly-L-aspartic acid as a carrier for doxorubicin: a comparative in vivo study of free and polymer-bound drug.

作者信息

Pratesi G, Savi G, Pezzoni G, Bellini O, Penco S, Tinelli S, Zunino F

出版信息

Br J Cancer. 1985 Dec;52(6):841-8. doi: 10.1038/bjc.1985.267.

Abstract

The synthetic polypeptide, poly-L-aspartic acid (PAA, mol. wt = 20,000) has been used as a macromolecular carrier for doxorubicin. The drug may be released in vivo through hydrolysis of the ester linkage formed between the carboxyl groups of the polymer and the drug side chain. PAA has been found to be a suitable carrier since it is a soluble, biodegradable, multivalent and nontoxic polymer. The toxicity and the therapeutic efficacy of free and polymer-linked doxorubicin have been evaluated in normal and tumour-bearing mice, using a variety of experimental tumour systems. In studies on single and multiple drug administration, the results indicated that the polymeric derivative of doxorubicin had approximately 3-fold lower toxicity than did free drug. In addition, the severity of specific toxic effects, including cardio- and vesicant toxicity, were appreciably reduced following conjugation to PAA. The doxorubicin-PAA conjugate gave similar or rather greater therapeutic effects than free drug at less toxic doses. This effect, more evident in the highly sensitive tumours, suggests an improvement of the therapeutic index of the polymer-linked drug.

摘要

合成多肽聚-L-天冬氨酸(PAA,分子量 = 20,000)已被用作阿霉素的大分子载体。药物可通过聚合物羧基与药物侧链之间形成的酯键水解在体内释放。已发现PAA是一种合适的载体,因为它是一种可溶、可生物降解、多价且无毒的聚合物。使用多种实验性肿瘤系统,在正常小鼠和荷瘤小鼠中评估了游离阿霉素和与聚合物连接的阿霉素的毒性及治疗效果。在单次和多次给药研究中,结果表明阿霉素的聚合物衍生物毒性比游离药物低约3倍。此外,与PAA偶联后,包括心脏毒性和发泡剂毒性在内的特定毒性作用的严重程度明显降低。阿霉素-PAA偶联物在较低毒性剂量下产生的治疗效果与游离药物相似或更强。这种效应在高敏感性肿瘤中更为明显,表明与聚合物连接的药物的治疗指数有所提高。

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