Piperazine Oxadiazole Inhibitors of Acetyl-CoA Carboxylase

Matthew P. Bourbeau,Aaron C. Siegmund,John G. Allen,Hong Shu,Christopher Fotsch,Michael D. Bartberger,Ki-Won Kim,Renee Komorowski,Melissa Graham,James Busby,Minghan Wang,James Meyer,Yang Xu,Kevin Salyers,Mark R. Fielden,Murielle M. Véniant,Wei Gu

Piperazine Oxadiazole Inhibitors of Acetyl-CoA Carboxylase

2013

Matthew P. Bourbeau
Aaron C. Siegmund
John G. Allen
Hong Shu
Christopher Fotsch
Michael D. Bartberger
Ki-Won Kim
Renee Komorowski
Melissa Graham
James Busby
Minghan Wang
James Meyer
Yang Xu
Kevin Salyers
Mark R. Fielden
Murielle M. Véniant
Wei Gu

Acetyl-CoA carboxylase (ACC) is a target of interest for the treatment of metabolic syndrome. Starting from a biphenyloxadiazole screening hit, a series of piperazine oxadiazole ACC inhibitors was developed. Initial pharmacokinetic liabilities of the piperazine oxadiazoles were overcome by blocking predicted sites of metabolism, resulting in compounds with suitable properties for further in vivo studies. Compound 26 was shown to inhibit malonyl-CoA production in an in vivo pharmacodynamic assay and was advanced to a long-term efficacy study. Prolonged dosing with compound 26 resulted in impaired glucose tolerance in diet-induced obese (DIO) C57BL6 mice, an unexpected finding.

Keywords:

Acetyl-CoA carboxylase
Biochemistry
Metabolism
In vivo
Pharmacodynamics
Oxadiazole
Organic chemistry
Pyruvate carboxylase
Piperazine
Chemistry
Pharmacology
Pharmacokinetics

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations