Discovery and SAR of a novel series of potent, CNS penetrant M4 PAMs based on a non-enolizable ketone core: Challenges in disposition.

Michael R. Wood,Meredith J. Noetzel,James C. Tarr,Alice L. Rodriguez,Atin Lamsal,Sichen Chang,Jarrett J. Foster,Emery Smith,Peter Chase,Peter Hodder,Darren W. Engers,Colleen M. Niswender,Nicholas J. Brandon,Michael W. Wood,Mark E. Duggan,P. Jeffrey Conn,Thomas M. Bridges,Craig W. Lindsley

Discovery and SAR of a novel series of potent, CNS penetrant M4 PAMs based on a non-enolizable ketone core: Challenges in disposition.

2016

Michael R. Wood
Meredith J. Noetzel
James C. Tarr
Alice L. Rodriguez
Atin Lamsal
Sichen Chang
Jarrett J. Foster
Emery Smith
Peter Chase
Peter Hodder
Darren W. Engers
Colleen M. Niswender
Nicholas J. Brandon
Michael W. Wood
Mark E. Duggan
P. Jeffrey Conn
Thomas M. Bridges
Craig W. Lindsley

This Letter describes the chemical optimization of a novel series of M4 PAMs based on a non-enolizable ketone core, identified from an MLPCN functional high-throughput screen. The HTS hit was potent, selective and CNS penetrant; however, the compound was highly cleared in vitro and in vivo. SAR provided analogs for which M4 PAM potency and CNS exposure were maintained; yet, clearance remained high. Metabolite identification studies demonstrated that this series was subject to rapid, and near quantitative, reductive metabolism to the corresponding secondary alcohol metabolite that was devoid of M4 PAM activity.

Keywords:

Biochemistry
Structure–activity relationship
In vivo
Drug discovery
Ketone
Chemistry
Metabolite
In vitro
Allosteric regulation
Penetrant (mechanical, electrical, or structural)

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