Non-peptide angiotensin II receptor antagonists. 2. Design, synthesis, and biological activity of N-substituted (phenylamino) phenylacetic acids and acyl sulfonamides

DS Dhanoa, SW Bagley, RSL Chang…

Index: Dhanoa, Daljit S.; Bagley, Scott W.; Chang, Raymond S. L.; Lotti, Victor J.; Chen, Tsing-Bau; et al. Journal of Medicinal Chemistry, 1993 , vol. 36, # 26 p. 4239 - 4249

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Citation Number: 22

Abstract

Inhibition of the renin-angiotensin system (RAS) by angiotensin I1 (AII) receptor antagonists continues to be the most active area of drug discovery for the treatment of hypertension and congestive heart fail~ re.~ Recently, we have described a new class of potent AT1-selective AI1 receptor antagonists derived from N-substituted indoles and dihydr~ indoles.~ In our continuing efforts to discover a structurally distinct class of AI1 antagonists, we became ...

 Related Synthetic Route
Ethanol Structure

64-17-5

Ethanol

2,5-Difluorophenylacetic acid Structure

85068-27-5

2,5-Difluorophe...

~94%

ETHYL(2,5-DIFLUOROPHENYL)ACETATE Structure

662138-60-5

ETHYL(2,5-DIFLU...

3-Methyl-4-nitrobenzoic acid Structure

3113-71-1

3-Methyl-4-nitr...

~97%

(3-METHYL-4-NITROPHENYL)METHANOL Structure

80866-75-7

(3-METHYL-4-NIT...

(3-METHYL-4-NITROPHENYL)METHANOL Structure

80866-75-7

(3-METHYL-4-NIT...

~92%

3-METHYL-4-NITROBENZYL BROMIDE Structure

141281-38-1

3-METHYL-4-NITR...


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