Author/Authors :
Rui Liang، نويسنده , , Lauren Abrardo، نويسنده , , Edward J. Brady، نويسنده , , Mari Rios Candelore، نويسنده , , Victor Ding، نويسنده , , Richard Saperstein، نويسنده , , Laurie M. Tota، نويسنده , , Michael Wright، نويسنده , , Steve Mock، نويسنده , , Constantin Tamvakopolous، نويسنده , , Sharon Tong، نويسنده , , Song Zheng، نويسنده , , Bei B. Zhang، نويسنده , , James R. Tata، نويسنده , , Emma R. Parmee، نويسنده ,
Abstract :
A series of conformationally constrained tri-substituted ureas were synthesized, and their potential as glucagon receptor antagonists was evaluated. This effort resulted in the identification of compound 4a, which had a binding IC50 of 4.0 nM and was shown to reduce blood glucose levels at 3 mg/kg in glucagon-challenged mice containing a humanized glucagon receptor. Compound 4a was efficacious in correcting hyperglycemia induced by a high fat diet in transgenic mice at an oral dose as low as 3 mg/kg.
Keywords :
Hyperglycemia , Diabetes , Glucagon receptor , glucagon , Glucagon receptor antagonist , glucose
