Literature

Abstract

The activity of different analogs of pyrazinamide on Mycobacterium tuberculosis fatty acid synthase type I (FASI) in replicating bacilli was studied. Palmitic acid biosynthesis was diminished by 96% in bacilli treated with n-propyl pyrazinoate, 94% in bacilli treated with 5-chloro-pyrazinamide, and 97% in bacilli treated with pyrazinoic acid, the pharmacologically active agent of pyrazinamide. We conclude that the minimal structure of pyrazine ring with an acyl group is sufficient for FASI inhibition and antimycobacterial activity.

DOI： 10.1128/aac.01369-06

Pyrazinoic Acid and Its n -Propyl Ester Inhibit Fatty Acid Synthase Type I in Replicating Tubercle Bacilli

Antimicrobial Agents and Chemotherapy 2007.0

Inhibition of Isolated Mycobacterium tuberculosis Fatty Acid Synthase I by Pyrazinamide Analogs

Antimicrobial Agents and Chemotherapy 2007.0

Pyrazinamide, but not pyrazinoic acid, is a competitive inhibitor of NADPH binding to Mycobacterium tuberculosis fatty acid synthase I

Bioorganic & Medicinal Chemistry Letters 2011.0

Antimycobacterial activity of a series of pyrazinoic acid esters

Journal of Medicinal Chemistry 1992.0

Pyrazinoic Acid Esters with Broad Spectrum in Vitro Antimycobacterial Activity

Journal of Medicinal Chemistry 1995.0

Synthesis and Antimycobacterial Activity of Pyrazine and Quinoxaline Derivatives