Optimization of Novel Aza-benzimidazolone mGluR2 PAMs with Respect to LLE and PK Properties and Mitigation of CYP TDI

Joseph E. Pero,Michael A. Rossi,Michael J. Kelly,Hannah D. G. F. Lehman,Mark E. Layton,Robert M. Garbaccio,Julie A. OBrien,Brian C. Magliaro,Jason M. Uslaner,Sarah L. Huszar,Kerry L. Fillgrove,Cuyue Tang,Yuhsin Kuo,Leo A. Joyce,Edward C. Sherer,Marlene A. Jacobson

Optimization of Novel Aza-benzimidazolone mGluR2 PAMs with Respect to LLE and PK Properties and Mitigation of CYP TDI

2016

Joseph E. Pero
Michael A. Rossi
Michael J. Kelly
Hannah D. G. F. Lehman
Mark E. Layton
Robert M. Garbaccio
Julie A. OBrien
Brian C. Magliaro
Jason M. Uslaner
Sarah L. Huszar
Kerry L. Fillgrove
Cuyue Tang
Yuhsin Kuo
Leo A. Joyce
Edward C. Sherer
Marlene A. Jacobson

Investigation of a novel amino-aza-benzimidazolone structural class of positive allosteric modulators (PAMs) of metabotropic glutamate receptor 2 (mGluR2) identified [2.2.2]-bicyclic amine 12 as an intriguing lead structure due to its promising physicochemical properties and lipophilic ligand efficiency (LLE). Further optimization led to chiral amide 18, which exhibited strong in vitro activity and attractive pharmacokinetic (PK) properties. Hypothesis-driven target design identified compound 21 as a potent, highly selective, orally bioavailable mGluR2 PAM, which addressed a CYP time-dependent inhibition (TDI) liability of 18, while maintaining excellent drug-like properties with robust in vivo activity in a clinically validated model of antipsychotic potential.

Keywords:

Biochemistry
Pharmacology
Metabotropic glutamate receptor 2
Amide
Ligand efficiency
Allosteric regulation
Pharmacokinetics
Metabotropic glutamate receptor
Chemistry
Stereochemistry
In vivo
Amine gas treating

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