Metabolic activation of N-thiazol-2-yl benzamide as glucokinase activators: Impacts of glutathione trapping on covalent binding |
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Authors: | Tomoharu Iino Noriaki Hashimoto Takuro Hasegawa Masato Chiba Jun-ichi Eiki Teruyuki Nishimura |
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Affiliation: | Banyu Tsukuba Research Institute, Banyu Pharmaceutical Co. Ltd, Japan |
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Abstract: | Glucokinase activators (GKAs) are currently under investigation as potential antidiabetic agents by many pharmaceutical companies. Most of GKAs reported previously possess N-aminothiazol-2-yl amide moiety in their structures because the aminothiazole moiety interacts with glucokinase (GK) and shows strong GK activation. During the development of N-aminothiazol-2-yl amide derivatives, we identified a bioactivation and metabolic liability of 2-aminothizole substructure of GKA 3 by assessing covalent binding, metabolites in liver microsomes and glutathione (GSH) trap assay. |
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