San Martin, LoretoCerda, FabianJin, ChunyangJimenez, VeronicaYevenes, Gonzalo E.Hernandez, TaniaNova, DanielaFuentealba, JorgeAguayo, Luis G.Guzman, Leonardo2023-09-262023-09-262016-09Journal of Biological Chemistry. Volume 291, Issue 36, Pages 18791 - 18798. 2 September 20160021-9258https://repositorio.unab.cl/xmlui/handle/ria/53333Indexación: Scopus.The acute intoxicating effects of ethanol in the central nervous system result from the modulation of several molecular targets. It is widely accepted that ethanol enhances the activity of the glycine receptor (GlyR), thus enhancing inhibitory neurotransmission, leading to motor effects, sedation, and respiratory depression. We previously reported that small peptides interfered with the binding of Gβγ to the GlyR and consequently inhibited the ethanol-induced potentiation of the receptor. Now, using virtual screening, we identified a subset of small molecules capable of interacting with the binding site of Gβγ. One of these compounds, M554, inhibited the ethanol potentiation of the GlyR in both evoked currents and synaptic transmission in vitro. When this compound was tested in vivo in mice treated with ethanol (1–3.5 g/kg), it was found to induce a faster recovery of motor incoordination in rotarod experiments and a shorter sedative effect in loss of righting reflex assays. This study describes a novel molecule that might be relevant for the design of useful therapeutic compounds in the treatment of acute alcohol intoxication.enAlcoholG ProteinGlycine ReceptorMolecular PharmacologySmall MoleculeGβγArtículoAtribution 4.0 International (CC BY 4.0)10.1074/jbc.M116.740555