Potent and orally active ET_A selective antagonists with 5,7-diarylcyclopenteno[1,2-b]pyridine-6-carboxylic acid structures

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• 作者：Yoshizumi ; Takashi ; Takahashi ; Hirobumi ; Ohtake ; Norikazu ; Jona ; Hideki ; Sato ; Yoshiyuki ; Kishino ; Hiroyuki ; et. al.
• 刊名：Bioorganic and Medicinal Chemistry
• 出版年：2004
• 出版时间：May 1, 2004
• 年：2004
• 卷：12
• 期：9
• 页码：2139-2150
• 全文大小：373 K

文摘

The synthesis and structure–activity relationships of a series of 5,7-diarylcyclopenteno[1,2-b]pyridine-6-carboxylic acids are described. Our efforts have been focused on modification of the aryl ring at the 5-position and the alkyl substituent at the 2-position of the bottom 4-methoxyphenyl ring in an effort to develop orally available ET_A selective antagonists with safer profiles in terms of the P-450 enzyme inhibitory activity. Incorporation of a hydroxymethyl group as an alkyl substituent in methylenedioxyphenyl and 6-dihydrobenzofuran derivatives led to the identification of orally bioavailable ET_A selective antagonists 1f and 7f. These compounds also showed not only excellent binding affinity (IC₅₀<0.10nM, more than 800-fold selectivity for the ET_A receptor over the ET_B receptor) but also sufficient oral bioavailability, 48 % and 56 % , respectively, in rats. Furthermore, these compounds did not exhibit either competitive or mechanism-based inhibition of human cytochrome P450 enzymes.