Design and Synthesis of mGlu2 NAMs with Improved Potency and CNS Penetration Based on a Truncated Picolinamide Core

Katrina A. Bollinger,Andrew S. Felts,Christopher J. Brassard,Julie L. Engers,Alice L. Rodriguez,Rebecca L. Weiner,Hyekyung P. Cho,Sichen Chang,Michael Bubser,Carrie K. Jones,Anna L. Blobaum,Colleen M. Niswender,P. Jeffrey Conn,Kyle A. Emmitte,Craig W. Lindsley

Design and Synthesis of mGlu2 NAMs with Improved Potency and CNS Penetration Based on a Truncated Picolinamide Core

2017

Katrina A. Bollinger
Andrew S. Felts
Christopher J. Brassard
Julie L. Engers
Alice L. Rodriguez
Rebecca L. Weiner
Hyekyung P. Cho
Sichen Chang
Michael Bubser
Carrie K. Jones
Anna L. Blobaum
Colleen M. Niswender
P. Jeffrey Conn
Kyle A. Emmitte
Craig W. Lindsley

Herein, we detail the optimization of the mGlu2 negative allosteric modulator (NAM), VU6001192, by a reductionist approach to afford a novel, simplified mGlu2 NAM scaffold. This new chemotype not only affords potent and selective mGlu2 inhibition, as exemplified by VU6001966 (mGlu2 IC50 = 78 nM, mGlu3 IC50 > 30 μM), but also excellent central nervous system (CNS) penetration (Kp = 1.9, Kp,uu = 0.78), a feature devoid in all previously disclosed mGlu2 NAMs (Kps ≈ 0.3, Kp,uus ≈ 0.1). Moreover, this series, based on overall properties, represents an exciting lead series for potential mGlu2 PET tracer development.

Keywords:

Pharmacology
Biochemistry
Allosteric modulator
Potency
IC50
Chemotype
Chemistry
Stereochemistry
Penetration (firestop)
pet tracer
cns penetration

Correction
Source
Cite
Save
Machine Reading By IdeaReader

References

Citations