Strategies to Mitigate the Bioactivation of 2-Anilino-7-Aryl-Pyrrolo[2,1-f][1,2,4]triazines: Identification of Orally Bioavailable, Efficacious ALK Inhibitors

Eugen F. Mesaros,Tho V. Thieu,Gregory J. Wells,Craig A. Zificsak,Jason C. Wagner,Henry J. Breslin,Rabindranath Tripathy,James L. Diebold,Robert J. McHugh,Ashley T. Wohler,Matthew R. Quail,Weihua Wan,Lihui Lu,Zeqi Huang,Mark S. Albom,Thelma S. Angeles,Kevin J. Wells-Knecht,Lisa D. Aimone,Mangeng Cheng,Mark A. Ator,Gregory R. Ott,Bruce D. Dorsey

Strategies to Mitigate the Bioactivation of 2-Anilino-7-Aryl-Pyrrolo[2,1-f][1,2,4]triazines: Identification of Orally Bioavailable, Efficacious ALK Inhibitors

2012

Chemical strategies to mitigate cytochrome P450-mediated bioactivation of novel 2,7-disubstituted pyrrolo[2,1-f][1,2,4]triazine ALK inhibitors are described along with synthesis and biological activity. Piperidine-derived analogues showing minimal microsomal reactive metabolite formation were discovered. Potent, selective, and metabolically stable ALK inhibitors from this class were identified, and an orally bioavailable compound (32) with antitumor efficacy in ALK-driven xenografts in mouse models was extensively characterized.

Keywords:

Aryl
Biochemistry
Cytochrome
Metabolite
Triazine
Organic chemistry
Bioavailability
Biological activity
Chemistry
reactive metabolite
Microsome
Stereochemistry

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