Structure-activity relationships of 1,5-biaryl pyrroles as EP1 receptor antagonists

Structure-activity relationships of 1,5-biaryl pyrroles as EP1 receptor antagonists

The preliminary SAR of a series of novel 1,5-biaryl pyrrole EP1 receptor antagonists derived from compound 1 is described. Replacement of the benzyl group of 1 with isosteric groups was investigated. The most effective replacement was found to be the isobutyl group. The cyclopentylmethyl and cyclohe...

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Veröffentlicht in:Bioorganic & medicinal chemistry letters 2006-07, Vol.16 (14), p.3657-3662
Hauptverfasser: HALL, Adrian, ATKINSON, Stephen, HEALY, Mark P, JOHNSON, Matthew R, MICHEL, Anton D, NAYLOR, Alan, NOVELLI, Riccardo, SPALDING, David J, TANG, Sac P, BROWN, Susan H, CHESSELL, Iain P, CHOWDHURY, Anita, CLAYTON, Nicholas M, COLEMAN, Tanya, GIBLIN, Gerard M. P, GLEAVE, Robert J, HAMMOND, Beverley
Format: Artikel
Sprache:eng
Schlagworte:
Analgesics - pharmacology
Animals
Benzoates - chemical synthesis
Benzoates - pharmacology
Biological and medical sciences
Biological Availability
Bones, joints and connective tissue. Antiinflammatory agents
Cyclohexanes - chemistry
Cyclopentanes - chemistry
Inflammation - drug therapy
Inflammation - pathology
Ligands
Medical sciences
Pain - drug therapy
Pain - pathology
Pharmacology. Drug treatments
Pyrroles - chemistry
Pyrroles - pharmacology
Rats
Receptors, Prostaglandin E - antagonists & inhibitors
Receptors, Prostaglandin E, EP1 Subtype
Structure-Activity Relationship
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Zusammenfassung:The preliminary SAR of a series of novel 1,5-biaryl pyrrole EP1 receptor antagonists derived from compound 1 is described. Replacement of the benzyl group of 1 with isosteric groups was investigated. The most effective replacement was found to be the isobutyl group. The cyclopentylmethyl and cyclohexylmethyl groups were also effective benzyl replacements. The cyclohexylmethyl derivative 19 demonstrated the lowest metabolic clearance within this series. In addition, several high affinity substituted benzyl analogues were also identified. Compound 39 was found to have good bioavailability in rats and demonstrated efficacy in the established FCA preclinical model of inflammatory pain with a calculated ED50 of 9.2mg/kg.
ISSN:0960-894X
1464-3405
DOI:10.1016/j.bmcl.2006.04.073