Challenges in the development of an M4 PAM preclinical candidate: The discovery, SAR, and in vivo characterization of a series of 3-aminoazetidine-derived amides

James C. Tarr,Michael R. Wood,Meredith J. Noetzel,Jeanette L. Bertron,Rebecca L. Weiner,Alice L. Rodriguez,Atin Lamsal,Frank W. Byers,Sichen Chang,Hyekyung P. Cho,Carrie K. Jones,Colleen M. Niswender,Michael W. Wood,Nicholas J. Brandon,Mark E. Duggan,P. Jeffrey Conn,Thomas M. Bridges,Craig W. Lindsley

Challenges in the development of an M4 PAM preclinical candidate: The discovery, SAR, and in vivo characterization of a series of 3-aminoazetidine-derived amides

2017

James C. Tarr
Michael R. Wood
Meredith J. Noetzel
Jeanette L. Bertron
Rebecca L. Weiner
Alice L. Rodriguez
Atin Lamsal
Frank W. Byers
Sichen Chang
Hyekyung P. Cho
Carrie K. Jones
Colleen M. Niswender
Michael W. Wood
Nicholas J. Brandon
Mark E. Duggan
P. Jeffrey Conn
Thomas M. Bridges
Craig W. Lindsley

Abstract This letter details the continued chemical optimization of a novel series of M 4 positive allosteric modulators (PAMs) based on a 5-amino-thieno[2,3- c ]pyridazine core by incorporating a 3-amino azetidine amide moiety. The analogs described within this work represent the most potent M 4 PAMs reported for this series to date. The SAR to address potency, clearance, subtype selectivity, CNS exposure, and P-gp efflux are described. This work culminated in the discovery of VU6000918, which demonstrated robust efficacy in a rat amphetamine-induced hyperlocomotion reversal model at a minimum efficacious dose of 0.3 mg/kg.

Keywords:

Potency
In vivo
Biochemistry
Allosteric regulation
Chemistry
Pyridazine
Azetidine
Efflux
subtype selectivity
Stereochemistry
Moiety

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