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dc.rights.licenseReconocimiento-NoComercial-SinObraDerivada. (CC BY-NC-ND)es
dc.contributor.authorTrias, Emilianoes
dc.contributor.authorIbarburu, Sofíaes
dc.contributor.authorBarreto-Núñez, Rominaes
dc.contributor.authorBabdor, Joëles
dc.contributor.authorMaciel, Thiago T.es
dc.contributor.authorGuillo, Matthiases
dc.contributor.authorGros, Laurentes
dc.contributor.authorDubreuil, Patricees
dc.contributor.authorDíaz-Amarilla, Pabloes
dc.contributor.authorCassina, Patriciaes
dc.contributor.authorMartínez-Palma, Lauraes
dc.contributor.authorMoura, Ivan C.es
dc.contributor.authorBeckman, Joseph S.es
dc.contributor.authorHermine, Olivieres
dc.contributor.authorBarbeito, Luises
dc.date.accessioned2019-10-25T14:41:04Z-
dc.date.available2019-10-25T14:41:04Z-
dc.date.issued2016-
dc.identifier.urihttp://hdl.handle.net/20.500.12381/169-
dc.description.abstractBackground: In the SOD1G93A mutant rat model of amyotrophic lateral sclerosis (ALS), neuronal death and rapid paralysis progression are associated with the emergence of activated aberrant glial cells that proliferate in the degenerating spinal cord. Whether pharmacological downregulation of such aberrant glial cells will decrease motor neuron death and prolong survival is unknown. We hypothesized that proliferation of aberrant glial cells is dependent on kinase receptor activation, and therefore, the tyrosine kinase inhibitor masitinib (AB1010) could potentially control neuroinflammation in the rat model of ALS. Methods: The cellular effects of pharmacological inhibition of tyrosine kinases with masitinib were analyzed in cell cultures of microglia isolated from aged symptomatic SOD1G93A rats. To determine whether masitinib prevented the appearance of aberrant glial cells or modified post-paralysis survival, the drug was orally administered at 30 mg/kg/day starting after paralysis onset. Results: We found that masitinib selectively inhibited the tyrosine kinase receptor colony-stimulating factor 1R (CSF-1R) at nanomolar concentrations. In microglia cultures from symptomatic SOD1G93A spinal cords, masitinib prevented CSF-induced proliferation, cell migration, and the expression of inflammatory mediators. Oral administration of masitinib to SOD1G93A rats starting after paralysis onset decreased the number of aberrant glial cells, microgliosis, and motor neuron pathology in the degenerating spinal cord, relative to vehicle-treated rats. Masitinib treatment initiated 7 days after paralysis onset prolonged post-paralysis survival by 40 %. Conclusions: These data show that masitinib is capable of controlling microgliosis and the emergence/expansion of aberrant glial cells, thus providing a strong biological rationale for its use to control neuroinflammation in ALS. Remarkably, masitinib significantly prolonged survival when delivered after paralysis onset, an unprecedented effect in preclinical models of ALS, and therefore appears well-suited for treating ALS.es
dc.description.sponsorshipAgencia Nacional de Investigación e Innovaciónes
dc.format.extent12 p.es
dc.language.isoenges
dc.publisherBMCes
dc.rightsAcceso abiertoes
dc.sourceJournal of Neuroinflammation. 2016, 13:177es
dc.subjectALSes
dc.subjectAberrant glial cellses
dc.subjectNeurodegenerationes
dc.subjectMasitinibes
dc.subjectM-CSFes
dc.titlePost-paralysis tyrosine kinase inhibition with masitinib abrogates neuroinflammation and slows disease progression in inherited amyotrophic lateral sclerosises
dc.typeArtículoes
dc.subject.aniiCiencias Médicas y de la Saludes
dc.subject.aniiBiotecnología de la Saludes
dc.identifier.aniiFCE_1_2011_1_7342es
dc.type.versionPublicadoes
dc.identifier.doihttp://dx.doi.org/10.1186/s12974-016-0620-9-
dc.anii.institucionresponsableInstitut Pasteur de Montevideoes
Aparece en las colecciones: Institut Pasteur de Montevideo

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