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新型注射用聚(癸二酸-蓖麻油酸)聚合物中顺铂和紫杉醇的药代动力学和疗效研究。

Pharmacokinetic and efficacy study of cisplatin and paclitaxel formulated in a new injectable poly(sebacic-co-ricinoleic acid) polymer.

机构信息

BioLineRx Ltd., Jerusalem, Israel.

出版信息

Eur J Pharm Biopharm. 2012 Sep;82(1):85-93. doi: 10.1016/j.ejpb.2012.06.004. Epub 2012 Jun 23.

DOI:10.1016/j.ejpb.2012.06.004
PMID:22732267
Abstract

Injectable biodegradable polymer poly(sebacic-co-ricinoleic acid), P(SA-RA) is currently under development for intratumoral (IT) delivery of drugs for treating solid tumors. This study presents formulation development, pharmacokinetic and efficacy studies of two anticancer drugs (cisplatin and paclitaxel) formulated with P(SA-RA) polymer. In pharmacokinetic study, systemic exposure and pharmacokinetic parameters of cisplatin/paclitaxel following single intravenous (IV) or subcutaneous (SC) doses of cisplatin/paclitaxel was compared with intramuscular (IM) or SC doses of cisplatin/paclitaxel formulated with P(SA-RA) polymer in male CD rat. Simultaneously, the tumor reduction effect and toxicity for these formulations were evaluated in human FaDu head and neck tumor xenograft subcutaneous nude mouse model. Pharmacokinetic data reflect the lower maximal concentrations and sustained release of polymer-cisplatin/paclitaxel formulations compared to standard cisplatin/paclitaxel administration. Regarding efficacy study, a single IT or near the tumor injection (NT) of polymer-paclitaxel or polymer-cisplatin formulation significantly reduced the tumor size, compared to the standard paclitaxel or cisplatin treatments. No death or toxicity and no effect on body weight as well as macroscopic and/or microscopic changes in or near the injected area were observed, proving biocompatibility and acceptability of polymer-formulations. In conclusion, the developed formulation demonstrated controlled release and significant efficacy in delivering these agents and exhibit potential for further clinical development.

摘要

可注射生物降解聚合物聚(癸二酸-蓖麻油酸),P(SA-RA),目前正在开发用于治疗实体瘤的瘤内(IT)药物输送。本研究介绍了两种抗癌药物(顺铂和紫杉醇)与 P(SA-RA)聚合物制剂的配方开发、药代动力学和疗效研究。在药代动力学研究中,比较了顺铂/紫杉醇单静脉(IV)或皮下(SC)给药与 P(SA-RA)聚合物制剂的顺铂/紫杉醇肌内(IM)或 SC 给药后顺铂/紫杉醇的全身暴露和药代动力学参数在雄性 CD 大鼠中。同时,在人 FaDu 头颈部肿瘤异种移植皮下裸鼠模型中评估了这些制剂的肿瘤缩小效果和毒性。药代动力学数据反映了聚合物-顺铂/紫杉醇制剂的最大浓度和持续释放低于标准顺铂/紫杉醇给药。关于疗效研究,与标准紫杉醇或顺铂治疗相比,聚合物-紫杉醇或聚合物-顺铂制剂的单次 IT 或肿瘤附近(NT)注射显著减小了肿瘤大小。未观察到死亡或毒性,也未观察到体重以及注射部位或附近的宏观和/或微观变化,证明了聚合物制剂的生物相容性和可接受性。总之,所开发的制剂在递送这些药物方面表现出了控释和显著疗效,并显示出进一步临床开发的潜力。

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