前药
化学
代谢物
活性代谢物
生物利用度
生物化学
药理学
生物
作者
Jiapeng Li,Daniel Macedo de Melo Jorge,Weiwen Wang,Shuxin Sun,Tristan Frum,Yu-An Hang,Yueting Liu,Xingwu Zhou,Jingcheng Xiao,Xinwen Wang,Jason R. Spence,Christiane E. Wobus,Hao‐Jie Zhu
标识
DOI:10.1021/acs.jmedchem.4c00234
摘要
We assessed factors that determine the tissue-specific bioactivation of ProTide prodrugs by comparing the disposition and activation of remdesivir (RDV), its methylpropyl and isopropyl ester analogues (MeRDV and IsoRDV, respectively), the oral prodrug GS-621763, and the parent nucleotide GS-441524 (Nuc). RDV and MeRDV yielded more active metabolite remdesivir-triphosphate (RDV-TP) than IsoRDV, GS-621763, and Nuc in human lung cell models due to superior cell permeability and higher susceptivity to cathepsin A. Intravenous administration to mice showed that RDV and MeRDV delivered significantly more RDV-TP to the lung than other compounds. Nevertheless, all four ester prodrugs exhibited very low oral bioavailability (<2%), with Nuc being the predominant metabolite in blood. In conclusion, ProTides prodrugs, such as RDV and MeRDV, are more efficient in delivering active metabolites to the lung than Nuc, driven by high cell permeability and susceptivity to cathepsin A. Optimizing ProTides' ester structures is an effective strategy for enhancing prodrug activation in the lung.
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