Development of a more highly selective M1 antagonist from the continued optimization of the MLPCN Probe ML012

Bruce J. Melancon,Alexander P. Lamers,Thomas M. Bridges,Gary A. Sulikowski,Thomas J. Utley,Douglas J. Sheffler,Meredith J. Noetzel,Ryan D. Morrison,J. Scott Daniels,Colleen M. Niswender,Carrie K. Jones,P. Jeffrey Conn,Craig W. Lindsley,Michael R. Wood

Development of a more highly selective M1 antagonist from the continued optimization of the MLPCN Probe ML012

2012

Bruce J. Melancon
Alexander P. Lamers
Thomas M. Bridges
Gary A. Sulikowski
Thomas J. Utley
Douglas J. Sheffler
Meredith J. Noetzel
Ryan D. Morrison
J. Scott Daniels
Colleen M. Niswender
Carrie K. Jones
P. Jeffrey Conn
Craig W. Lindsley
Michael R. Wood

This Letter describes the continued optimization of an MLPCN probe molecule (ML012) through an iterative parallel synthesis approach. After exploring extensive modifications throughout the parent structure, we arrived at a more highly M1-selective antagonist, compound 13l (VU0415248). Muscarinic subtype selectivity across all five human and rat receptors for 13l, along with rat selectivity for the lead compound (ML012), is presented.

Keywords:

Lead compound
Parent structure
Molecular probe
Muscarinic acetylcholine receptor
Structure–activity relationship
Stereochemistry
Chemistry
Receptor
Biochemistry
highly selective
Antagonist
Selectivity

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