化学
前药
苯并噻唑
亲脂性
细胞毒性
细胞色素P450
硬脂酰辅酶A去饱和酶
生物化学
肿瘤细胞
酶
药理学
体外
癌症研究
生物
基因表达
基因
作者
Noelle S. Williams,Stephen S. Gonzales,Jacinth Naidoo,Giomar Rivera‐Cancel,Sukesh Voruganti,Prema L. Mallipeddi,Panayotis C. Theodoropoulos,Sophie Geboers,Hong Chen,Francisco Ortiz,Bruce A. Posner,Deepak Nijhawan,Joseph M. Ready
标识
DOI:10.1021/acs.jmedchem.0c00899
摘要
A series of N-acyl benzothiazoles shows selective and potent cytotoxicity against cancer cell lines expressing cytochrome P450 4F11. A prodrug form is metabolized by cancer cells into an active inhibitor of stearoyl-CoA desaturase (SCD). Substantial variation on the acyl portion of the inhibitors allowed the identification of (R)-27, which balanced potency, solubility, and lipophilicity to allow proof-of-concept studies in mice. The prodrugs were activated inside the tumor, where they can arrest tumor growth. Together, these observations offer promise that a tumor-activated prodrug strategy might exploit the essentiality of SCD for tumor growth, while avoiding toxicity associated with systemic SCD inhibition.
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