Seven cyclohexane-bearing C-glucoside derivatives(7,9,12,13 and 17-19) were designed and synthesized as SGLT2 inhibitors starting from a potent SGLT2 inhibitor we discovered in earlier work, (lS)-1-deoxy-l-[4-meth...Seven cyclohexane-bearing C-glucoside derivatives(7,9,12,13 and 17-19) were designed and synthesized as SGLT2 inhibitors starting from a potent SGLT2 inhibitor we discovered in earlier work, (lS)-1-deoxy-l-[4-methoxy-3-(trans-n-propylcyclohexyl)methylphenyl]-D-glucose(1).The in vitro and in vivo biological activities were evaluated by hSGLT2/hSGLTl inhibition and urinary glucose excretion (UGE),respectively.Among the synthesized compounds 12,the 6-deoxy derivative of 1 was the most active and selective SGLT2 inhibitor(IC_(50)= 1.4nmol/L against hSGLT2;selectivity = 1576).Compound 12 was a potent SGLT2 inhibitor,which could induce more urinary glucose than 1 and dapagliflozin in UGE.展开更多
基金Key Projects of Tianjin Science and Technology Support Plan(No.10ZCKFSH01300) for financial support
文摘Seven cyclohexane-bearing C-glucoside derivatives(7,9,12,13 and 17-19) were designed and synthesized as SGLT2 inhibitors starting from a potent SGLT2 inhibitor we discovered in earlier work, (lS)-1-deoxy-l-[4-methoxy-3-(trans-n-propylcyclohexyl)methylphenyl]-D-glucose(1).The in vitro and in vivo biological activities were evaluated by hSGLT2/hSGLTl inhibition and urinary glucose excretion (UGE),respectively.Among the synthesized compounds 12,the 6-deoxy derivative of 1 was the most active and selective SGLT2 inhibitor(IC_(50)= 1.4nmol/L against hSGLT2;selectivity = 1576).Compound 12 was a potent SGLT2 inhibitor,which could induce more urinary glucose than 1 and dapagliflozin in UGE.
