Discovery and Preclinical Development of AR453588 as an Anti-diabetic Glucokinase Activator

Ronald Jay Hinklin,Brian R. Baer,Steven A. Boyd,Mark D. Chicarelli,Kevin Ronald Condroski,Walter E. DeWolf,John Fischer,Michele Frank,Gary P. Hingorani,Patrice Lee,Nickolas A. Neitzel,Scott Alan Pratt,Ajay K. Singh,Francis X. Sullivan,Timothy M. Turner,Walter C. Voegtli,Eli M. Wallace,Lance A. Williams,Thomas Daniel Aicher

Discovery and Preclinical Development of AR453588 as an Anti-diabetic Glucokinase Activator

2019

Ronald Jay Hinklin
Brian R. Baer
Steven A. Boyd
Mark D. Chicarelli
Kevin Ronald Condroski
Walter E. DeWolf
John Fischer
Michele Frank
Gary P. Hingorani
Patrice Lee
Nickolas A. Neitzel
Scott Alan Pratt
Ajay K. Singh
Francis X. Sullivan
Timothy M. Turner
Walter C. Voegtli
Eli M. Wallace
Lance A. Williams
Thomas Daniel Aicher

Abstract Glucose flux through glucokinase (GK) controls insulin release from the pancreas in response to high levels of glucose. Flux through GK is also responsible for reducing hepatic glucose output. Since many individuals with type 2 diabetes appear to have an inadequacy or defect in one or both of these processes, identifying compounds that can activate GK could provide a therapeutic benefit. Herein we report the further structure activity studies of a novel series of glucokinase activators (GKA). These studies led to the identification of pyridine 72 as a potent GKA that lowered post-prandial glucose in normal C57BL/6J mice, and after 14d dosing in ob/ob mice.

Keywords:

Biochemistry
Chemistry
Glucokinase
Type 2 diabetes
Glucose output
Internal medicine
Pancreas
Glucokinase activator
Endocrinology
Insulin
ob/ob mouse
glucose flux
Diabetes mellitus
Pharmacology

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations