c-Abl tyrosine kinase down-regulation as target for memory improvement in Alzheimer's disease

dc.article.number16
dc.catalogadordfo
dc.contributor.authorLeon, Rilda
dc.contributor.authorGutierrez, Daniela A.
dc.contributor.authorPinto, Claudio
dc.contributor.authorMorales Acevedo, Cristián Gonzalo
dc.contributor.authorde la Fuente, Catalina
dc.contributor.authorRiquelme, Cristobal
dc.contributor.authorCortés Castro, Bastián Ignacio
dc.contributor.authorGonzalez-Martin, Adrian
dc.contributor.authorChamorro, David
dc.contributor.authorEspinosa, Nelson
dc.contributor.authorFuentealba Durand, Pablo José
dc.contributor.authorCancino Lobos, Gonzalo
dc.contributor.authorZanlungo Matsuhiro, Silvana
dc.contributor.authorDulcey, Andres E.
dc.contributor.authorMarugan, Juan J.
dc.contributor.authorRojas, Alejandra Alvarez
dc.date.accessioned2024-04-15T08:00:27Z
dc.date.available2024-04-15T08:00:27Z
dc.date.issued2023
dc.description.abstractBackgroundGrowing evidence suggests that the non-receptor tyrosine kinase, c-Abl, plays a significant role in the pathogenesis of Alzheimer's disease (AD). Here, we analyzed the effect of c-Abl on the cognitive performance decline of APPSwe/PSEN1 & UDelta;E9 (APP/PS1) mouse model for AD. MethodsWe used the conditional genetic ablation of c-Abl in the brain (c-Abl-KO) and pharmacological treatment with neurotinib, a novel allosteric c-Abl inhibitor with high brain penetrance, imbued in rodent's chow. ResultsWe found that APP/PS1/c-Abl-KO mice and APP/PS1 neurotinib-fed mice had improved performance in hippocampus-dependent tasks. In the object location and Barnes-maze tests, they recognized the displaced object and learned the location of the escape hole faster than APP/PS1 mice. Also, APP/PS1 neurotinib-fed mice required fewer trials to reach the learning criterion in the memory flexibility test. Accordingly, c-Abl absence and inhibition caused fewer amyloid plaques, reduced astrogliosis, and preserved neurons in the hippocampus. DiscussionOur results further validate c-Abl as a target for AD, and the neurotinib, a novel c-Abl inhibitor, as a suitable preclinical candidate for AD therapies.
dc.description.funderCentre for Social Conflict and Cohesion Studies (COES)
dc.description.funderAlberto Hurtado University
dc.description.funderFONDECYT
dc.description.funderANID
dc.fechaingreso.objetodigital2024-09-10
dc.fuente.origenWOS
dc.identifier.doi10.3389/fnagi.2023.1180987
dc.identifier.issn1663-4365
dc.identifier.pubmedidMEDLINE:34444039
dc.identifier.scopusidSCOPUS_ID:85134268346
dc.identifier.urihttps://doi.org/10.3389/fnagi.2023.1180987
dc.identifier.urihttps://repositorio.uc.cl/handle/11534/85086
dc.identifier.wosidWOS:001013034400001
dc.information.autorucEscuela de Ingeniería; Morales Acevedo Cristian Gonzalo; S/I; 177656
dc.information.autorucEscuela de Ingeniería; Cortes Castro Bastian Ignacio; S/I; 1087807
dc.information.autorucFacultad de Ciencias Biológicas; Fuentealba Durand Pablo Jose; 0000-0002-9679-4612; 19184
dc.information.autorucFacultad de Ciencias Biológicas; Cancino Lobos Gonzalo; S/I; 17709
dc.information.autorucFacultad de Ciencias Biológicas; Zanlungo Matsuhiro Silvana; 0000-0001-8383-9829; 72650
dc.issue.numero3
dc.language.isoen
dc.nota.accesoContenido completo
dc.pagina.final12
dc.pagina.inicio1
dc.revistaFrontiers in aging neuroscience
dc.rightsacceso abierto
dc.subjectc-Abl inhibitors
dc.subjectTyrosine kinases
dc.subjectAlzheimer's disease
dc.subjectMemory
dc.subjectHippocampi
dc.subject.ddc610
dc.subject.deweyMedicina y saludes_ES
dc.subject.ods03 Good Health and Well-being
dc.subject.odspa03 Salud y bienestar
dc.titlec-Abl tyrosine kinase down-regulation as target for memory improvement in Alzheimer's disease
dc.typeartículo
dc.volumen15
sipa.codpersvinculados177656
sipa.codpersvinculados1087807
sipa.codpersvinculados19184
sipa.codpersvinculados17709
sipa.codpersvinculados72650
sipa.indexWOS
sipa.trazabilidadWOS;2023-07-30
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