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Authordc.contributor.authorLaurido, Claudio 
Authordc.contributor.authorHernández, Alejandro es_CL
Authordc.contributor.authorPelissier Serrano, Teresa es_CL
Authordc.contributor.authorConstandil, Luis 
Admission datedc.date.accessioned2012-06-05T16:50:41Z
Available datedc.date.available2012-06-05T16:50:41Z
Publication datedc.date.issued2012
Cita de ítemdc.identifier.citationThe Scientific World Journal Volume 2012, Article ID 279147, 5 pageses_CL
Identifierdc.identifier.otherdoi:10.1100/2012/279147
Identifierdc.identifier.urihttps://repositorio.uchile.cl/handle/2250/128973
Abstractdc.description.abstractN-methyl-D-aspartic acid receptor (NMDAr) activation requires the presence ofD-serine, synthesized from L-serine by a pyridoxal 5 -phosphate-dependent serine racemase (SR). D-serine levels can be lowered by inhibiting the racemization of L-serine. Lserine- O-sulfate (LSOS) and L-erythro-3-hydroxyaspartate (LEHA), among others, have proven to be effective in reducing the D-serine levels in culture cells. It is tempting then to try these compounds in their effectiveness to decrease nociceptive levels in rat arthritic pain. We measured the C-reflex paradigm and wind-up potentiation in the presence of intrathecally injected LSOS (100 μg/10 μL) and LEHA (100 μg/10 μL) in normal and monoarthritic rats. Both compounds decreased the wind-up activity in normal and monoarthritic rats. Accordingly, all the antinociceptive effects were abolished when 300 μg/10 μL of D-serine were injected intrathecally. Since no in vivo results have been presented so far, this constitutes the first evidence that SR inhibitions lower the D-serine levels, thus decreasing the NMDAr activity and the consequent development and maintenance of chronic pain.es_CL
Patrocinadordc.description.sponsorshipFunded by Dicyt 021043-01LF, USACH; CEDENNA, Project FB-0807, and Fondecyt 1070115 and 1090476.es_CL
Lenguagedc.language.isoen_USes_CL
Publisherdc.publisherThe Scientific World Journales_CL
Títulodc.titleAntinociceptive Effect of Rat D-Serine Racemase Inhibitors, L-Serine-O-Sulfate, and L-Erythro-3-Hydroxyaspartate in an Arthritic Pain Modeles_CL
Document typedc.typeArtículo de revista


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