Abstract
Further optimization of the biaryl amide series via extensively exploring structure-activity relationships resulted in potent and subtype selective M(1) agonists exemplified by compounds 9a and 9j with good rat PK properties including CNS penetration. Synthesis, structure-activity relationships, subtype selectivity for M(1) over M(2-5), and DMPK properties of these novel compounds are described.
Copyright 2010 Elsevier Ltd. All rights reserved.
MeSH terms
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Amides / chemical synthesis*
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Amides / pharmacokinetics*
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Amides / pharmacology
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Animals
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Blood-Brain Barrier / metabolism
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Central Nervous System / metabolism
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Drug Discovery
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Hydrocarbons, Aromatic / chemical synthesis*
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Hydrocarbons, Aromatic / pharmacokinetics*
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Hydrocarbons, Aromatic / pharmacology
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Molecular Structure
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Rats
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Receptor, Muscarinic M1 / agonists*
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Structure-Activity Relationship
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Tissue Distribution
Substances
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Amides
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Hydrocarbons, Aromatic
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Receptor, Muscarinic M1