Full-profile pharmacokinetics, anticancer activity and toxicity of an extended release trivalent PEGylated irinotecan prodrug

伊立替康 前药 序号38 药代动力学 药理学 喜树碱 活性代谢物 化学 PEG比率 毒性 拓扑异构酶 医学 癌症 结直肠癌 内科学 体外 生物化学 经济 财务
作者
Shiwen Song,Dong Sun,Hong Wang,Jinliang Wang,Huijing Yan,Xuan Zhao,John Paul Fawcett,Xin Xu,Deqi Cai,Jingkai Gu
出处
期刊:Acta Pharmaceutica Sinica B [Elsevier BV]
卷期号:13 (8): 3444-3453 被引量:10
标识
DOI:10.1016/j.apsb.2023.01.011
摘要

Irinotecan is an anticancer topoisomerase I inhibitor that acts as a prodrug of the active metabolite, SN-38. Unfortunately, the limited utility of irinotecan is attributed to its pH-dependent stability, short half-life and dose-limiting toxicity. To address this problem, a novel trivalent PEGylated prodrug (PEG-[Irinotecan]3) has been synthesized and its full-profile pharmacokinetics, antitumor activity and toxicity compared with those of irinotecan. The results show that after intravenous administration to rats, PEG-[Irinotecan]3 undergoes stepwise loss of irinotecan to form PEG-[Irinotecan]3‒x (x = 1,2) and PEG-[linker] during which time the released irinotecan undergoes conversion to SN-38. As compared with conventional irinotecan, PEG-[Irinotecan]3 displays extended release of irinotecan and efficient formation of SN-38 with significantly improved AUC and half-life. In a colorectal cancer-bearing model in nude mice, the tumor concentrations of irinotecan and SN-38 produced by PEG-[Irinotecan]3 were respectively 86.2 and 2293 times higher at 48 h than produced by irinotecan. In summary, PEG-[Irinotecan]3 displays superior pharmacokinetic characteristics and antitumor activity with lower toxicity than irinotecan. This supports the view that PEG-[Irinotecan]3 is a superior anticancer drug to irinotecan and it has entered the phase II trial stage.
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