Synthesis and structure-activity relationships of thieno[2,3-b]pyrroles as antagonists of the GnRH receptor.

Jean Claude Arnould,Benedicte Delouvrie,Pascal Boutron,Al G. Dossetter,Kevin Michael Foote,Annie Hamon,Urs Hancox,Craig S. Harris,Mike Hutton,Maryannick Lamorlette,Zbigniew Stanley Matusiak

Synthesis and structure-activity relationships of thieno[2,3-b]pyrroles as antagonists of the GnRH receptor.

2007

Jean Claude Arnould
Benedicte Delouvrie
Pascal Boutron
Al G. Dossetter
Kevin Michael Foote
Annie Hamon
Urs Hancox
Craig S. Harris
Mike Hutton
Maryannick Lamorlette
Zbigniew Stanley Matusiak

Abstract A new class of small-molecule GnRH antagonists, the thieno[2,3- b ]pyrroles, was designed. Herein, the synthesis and structure–activity relationships are described. Substitution at the C4 position was investigated; during this study, it was observed that introducing piperazines and piperidines improved the physical properties of the compounds while retaining good in vitro potency. This exploration led to the discovery of amidopiperidines with improved pharmacokinetic properties.

Keywords:

Chemical synthesis
Small molecule
Antagonist
Biochemistry
Organic chemistry
Potency
Structure–activity relationship
Stereochemistry
Carboxamide
In vitro
Chemistry
Receptor
Gnrh receptor

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