Synthesis and in Vitro Antimycobacterial Activity of Some Pyridine and Pyrazinecarboxylic Acid Isosteres

Tuberculosis has been one of the most commonly encountered infectious diseases of humans throughout history. The discovery and introduction of effective Q:eatments in the 1940s resulted in a decline of the incidence of the disease until the 1980s, which marked a sharp turn in this trend with an increase in the number of reported cases in the world. The prevalence of mycobacterial infections in poorer nations and centers of urban decay, and especially in immunologically compromised patients indicates the need for new and better treatments. In this study, to contribute to the worldwide effort to discover more effective medications against mberculosis, 26 previously unreported compounds were synthesized and tested against Mycobacterium tuberculosis. The synthesized compounds were designed to act as bioisosteres or prodrugs of pyridine and pyrazinecarboxylic acid derivatives and contained acidic or neutral heteroor carbocyclic ring systems attached to pyridine or pyrazine rings at different positions. The synthesized ring systems included l,2,4-oxadiazole-5-ones, 1,2,4-thiadiazole-S-ones, l,2,4-oxadiazole-5-thiones, 1,3,4oxathiazoline-2-ones and cyclobutene-l,2-diones, which were documented in the literature to act as carboxylic acid isosteres or could act as prodrugs thereof. Pivaloyloxymethyl derivatives of the compounds were also prepared in order to increase their lipophilicity and therefore improve their bioavailability. The synthesized compounds were expected to be biotransformed by esterases or amidases to the active species after penetration of the mycobacterial cell wall. Biological and pharmacokinetic properties of the compounds were compared with the unmodified polar isosteres of