Artículo
WWOX P47T partial loss-of-function mutation induces epilepsy, progressive neuroinflammation, and cerebellar degeneration in mice phenocopying human SCAR12
Hussain, Tabish; Sanchez, Kevin; Crayton, Jennifer; Saha, Dhurjhoti; Jeter, Collene; Lu, Yue; Abba, Martín Carlos
; Seo, Ryan; Noebels, Jeffrey L.; Fonken, Laura; Aldaz, C. Marcelo
Fecha de publicación:
04/2023
Editorial:
Pergamon-Elsevier Science Ltd
Revista:
Progress In Neurobiology
ISSN:
0301-0082
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
WWOX gene loss-of-function (LoF) has been associated with neuropathologies resulting in developmental, epileptic, and ataxic phenotypes of varying severity based on the level of WWOX dysfunction. WWOX gene biallelic germline variant p.Pro47Thr (P47T) has been causally associated with a new form of autosomal recessive cerebellar ataxia with epilepsy and intellectual disability (SCAR12, MIM:614322). This mutation affecting the WW1 protein binding domain of WWOX, impairs its interaction with canonical proline-proline-X-tyrosine motifs in partner proteins. We generated a mutant knock-in mouse model of Wwox P47T mutation that phenocopies human SCAR12. WwoxP47T/P47T mice displayed epilepsy, profound social behavior and cognition deficits, and poor motor coordination, and unlike KO models that survive only for 1 month, live beyond 1 year of age. These deficits progressed with age and mice became practically immobile, suggesting severe cerebellar dysfunction. WwoxP47T/P47T mice brains revealed signs of progressive neuroinflammation with elevated astro-microgliosis that increased with age. Cerebellar cortex displayed significantly reduced molecular and granular layer thickness and a strikingly reduced number of Purkinje cells with degenerated dendrites. Transcriptome profiling from various brain regions of WW domain LoF mice highlighted widespread changes in neuronal and glial pathways, enrichment of bioprocesses related to neuroinflammation, and severe cerebellar dysfunction. Our results show significant pathobiological effects and potential mechanisms through which WWOX partial LoF leads to epilepsy, cerebellar neurodegeneration, neuroinflammation, and ataxia. Additionally, the mouse model described here will be a useful tool to understand the role of WWOX in common neurodegenerative conditions in which this gene has been identified as a novel risk factor.
Palabras clave:
ATAXIA
,
EPILEPSY
,
NEURODEGENERATION
,
NEUROINFLAMMATION
,
SCAR12
,
WWOX
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Identificadores
Colecciones
Articulos(CCT - LA PLATA)
Articulos de CTRO.CIENTIFICO TECNOL.CONICET - LA PLATA
Articulos de CTRO.CIENTIFICO TECNOL.CONICET - LA PLATA
Citación
Hussain, Tabish; Sanchez, Kevin; Crayton, Jennifer; Saha, Dhurjhoti; Jeter, Collene; et al.; WWOX P47T partial loss-of-function mutation induces epilepsy, progressive neuroinflammation, and cerebellar degeneration in mice phenocopying human SCAR12; Pergamon-Elsevier Science Ltd; Progress In Neurobiology; 223; 4-2023; 1-19
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