| Literature DB >> 24561669 |
Nuno Rodrigues1, Khalil Bennis2, Delphine Vivier1, Vanessa Pereira3, Franck C Chatelain4, Eric Chapuy3, Hemantkumar Deokar2, Jérôme Busserolles3, Florian Lesage4, Alain Eschalier5, Sylvie Ducki6.
Abstract
The TWIK-related K(+) channel, TREK-1, has recently emerged as an attractive therapeutic target for the development of a novel class of analgesic drugs. It has been reported that TREK-1 -/- mice were more sensitive than wild-type mice to painful stimuli, suggesting that activation of TREK-1 could result in pain inhibition. Here we report the synthesis of a series of substituted caffeate esters (12a-u) based on the hit compound CDC 2 (cinnamyl 3,4-dihydroxyl-α-cyanocinnamate). These analogs were evaluated for their ability to modulate TREK-1 channel by electrophysiology and for their in vivo antinociceptive activity (acetic acid induced-writhing assay) leading to the identification a series of novel molecules able to activate TREK-1 and displaying potent analgesic activity in vivo.Entities:
Keywords: Analgesic agents; Antinociceptive; Caffeate esters; Pain; QSAR; Structure–activity relationship study; TREK-1 channel
Mesh:
Substances:
Year: 2014 PMID: 24561669 DOI: 10.1016/j.ejmech.2014.01.049
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514