Identification of metabolites of the tryptase inhibitor CRA-9249: Observation of a metabolite derived from an unexpected hydroxylation pathway

…, T Mahajan, C O'Brian, EJ Shelton, D Sperandio…

文献索引：Yu, Walter; Dener, Jeffrey M.; Dickman, Daniel A.; Grothaus, Paul; Ling, Yun; Liu, Liang; Havel, Chris; Malesky, Kimberly; Mahajan, Tania; O'Brian, Colin; Shelton, Emma J.; Sperandio, David; Tong, Zhiwei; Yee, Robert; Mordenti, Joyce J. Bioorganic and Medicinal Chemistry Letters, 2006 , vol. 16, # 15 p. 4053 - 4058

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被引用次数: 2

摘要

The metabolites of the tryptase inhibitor CRA-9249 were identified after exposure to liver microsomes. CRA-9249 was found to be degraded rapidly in liver microsomes from rabbit, dog, cynomolgus monkey, and human, and less rapidly in microsomes from rat. The key metabolites included cleavage of an aryl ether, in addition to an unexpected hydroxylation of the amide side chain adjacent to the amide nitrogen. The chemical structures of both ...

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Synthesis of methyl (5S, 6R, 7E, 9E, 11Z, 13E, 15S)-16-(4-fl...

[Phillips, Eifion D.; Chang, Hui-Fang; Holmquist, Christopher R.; McCauley, John P. Bioorganic and Medicinal Chemistry Letters, 2003 , vol. 13, # 19 p. 3223 - 3226]