前药
化学
磷酰胺
体内
细胞毒性
药理学
体外
缺氧(环境)
吉西他滨
微粒体
生物化学
癌症
生物
有机化学
医学
内科学
氧气
生物技术
作者
Jian-Xin Duan,Hailong Jiao,Jacob A. Kaizerman,Timothy F. Stanton,James Evans,Lingyun Lan,Gustavo Lorente,Monica Banica,Don Jung,Jinwei Wang,Huaiyu Ma,Xiaoming Li,Zhijian Yang,Robert M. Hoffman,W. S. Ammons,Charles P. Hart,Mark Matteucci
摘要
A series of achiral hypoxia-activated prodrugs were synthesized on the basis of the DNA cross-linking toxin of the prodrug, ifosfamide. The hypoxia-selective cytotoxicity of several of the compounds was improved over previously reported racemic mixtures of chiral bioreductive phosphoramidate prodrugs. Prodrugs activated by 2-nitroimidazole reduction demonstrated up to 400-fold enhanced cytotoxicity toward H460 cells in culture under hypoxia versus their potency under aerobic conditions. Compounds were further assessed for their stability to cytochrome P450 metabolism using a liver microsome assay. The 2-nitroimidazole containing lead compound 3b (TH-302) was selectively potent under hypoxia and stable to liver microsomes. It was active in an in vivo MIA PaCa-2 pancreatic cancer orthotopic xenograft model as a monotherapy and demonstrated dramatic efficacy when used in combination with gemcitabine, extending survival with one of eight animals tumor free at day-44. Compound 3b has emerged as a promising antitumor agent that shows excellent in vivo efficacy and is currently being evaluated in the clinic.
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