Abstract
Previously we reported the discovery and initial optimization of a novel anthranilic acid derived class of antibacterial agents which suffered from extensive protein binding. This report describes efforts directed toward understanding the relationship of the acidity of the carboxylic acid with the extent of protein binding. The p K a of the acid was modified via the synthesis of a number of anthranilic acid analogs which vary the aromatic ring substituent at the 4-position. The p K a and HSA binding constants have been determined for each of the analogs. Our results indicate a correlation between p K a and HSA K d. The physical properties and antibacterial activities will be discussed as well as how these results help address the protein binding issue with this series of compounds.
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