Lead Optimization of Thiazolo[5,4‐c]piperidines: 3‐Cyclobutoxy Linker as a Key Spacer for H3R Inverse Agonists

Laurent Provins,Frédéric Denonne,Sylvain Celanire,Bernard Christophe,Sabine Defays,Christel Delaunoy,Marie-Laure Delporte,Thierry Demaude,Véronique Durieu,Michel Gillard,Delphine Hubert,Yves Lamberty,Geneviève Lorent,Anne Valade,Alain Vanbellinghen,Nathalie Van houtvin

Lead Optimization of Thiazolo[5,4‐c]piperidines: 3‐Cyclobutoxy Linker as a Key Spacer for H3R Inverse Agonists

2012

Laurent Provins
Frédéric Denonne
Sylvain Celanire
Bernard Christophe
Sabine Defays
Christel Delaunoy
Marie-Laure Delporte
Thierry Demaude
Véronique Durieu
Michel Gillard
Delphine Hubert
Yves Lamberty
Geneviève Lorent
Anne Valade
Alain Vanbellinghen
Nathalie Van houtvin

: The simpler, the better: H(3) histamine receptor (H(3)R) are of interest as therapeutic targets in cognitive and somnolence disorders. Here, lead optimization of H(3)R inverse agonists bearing a thiazolo[5,4-c]piperidine group gave rise to a clinical candidate with a much simpler unprecedented benzamide scaffold, displaying decreased hERG activity while maintaining high brain receptor occupancies.

Keywords:

Histamine H3 receptor
Linker
Inverse agonist
Organic chemistry
Stereochemistry
Chemistry
Histamine receptor
Benzamide
Combinatorial chemistry
Piperidine
brain receptor
hERG

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