Isatin replacements applied to the highly selective, muscarinic M1 PAM ML137: continued optimization of an MLPCN probe molecule.

Bruce J. Melancon,Michael S. Poslusney,Patrick R. Gentry,James C. Tarr,Douglas J. Sheffler,Margrith E. Mattmann,Thomas M. Bridges,Thomas J. Utley,J. Scott Daniels,Colleen M. Niswender,P. Jeffrey Conn,Craig W. Lindsley,Michael R. Wood

Isatin replacements applied to the highly selective, muscarinic M1 PAM ML137: continued optimization of an MLPCN probe molecule.

2013

Bruce J. Melancon
Michael S. Poslusney
Patrick R. Gentry
James C. Tarr
Douglas J. Sheffler
Margrith E. Mattmann
Thomas M. Bridges
Thomas J. Utley
J. Scott Daniels
Colleen M. Niswender
P. Jeffrey Conn
Craig W. Lindsley
Michael R. Wood

This Letter describes the continued optimization of an MLPCN probe molecule (ML137) with a focused effort on the replacement/modification of the isatin moiety present in this highly selective M1 PAM. A diverse range of structures were validated as viable replacements for the isatin, many of which engendered sizeable improvements in their ability to enhance the potency and efficacy of acetylcholine when compared to ML137. Muscarinic receptor subtype selectivity for the M1 receptor was also maintained.

Keywords:

Selectivity
Acetylcholine
Muscarinic acetylcholine receptor
Molecular probe
Moiety
Organic chemistry
Muscarinic acetylcholine receptor M1
Isatin
Stereochemistry
Allosteric regulation
Biochemistry
Chemistry
Molecule

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