Litcius/Paper detail

Shank2/3 double knockout-based screening of cortical subregions links the retrosplenial area to the loss of social memory in autism spectrum disorders

Débora Garrido, Stefania Beretta, Stefanie Grabrucker, Helen Friedericke Bauer, David Bayer, Carlo Sala, Chiara Verpelli, Francesco Roselli, Juergen Bockmann, Christian Proepper, Alberto Catanese, Tobias M. Boeckers

2022Molecular Psychiatry20 citationsDOIOpen Access PDF

Abstract

Members of the Shank protein family are master scaffolds of the postsynaptic architecture and mutations within the SHANK genes are causally associated with autism spectrum disorders (ASDs). We generated a Shank2-Shank3 double knockout mouse that is showing severe autism related core symptoms, as well as a broad spectrum of comorbidities. We exploited this animal model to identify cortical brain areas linked to specific autistic traits by locally deleting Shank2 and Shank3 simultaneously. Our screening of 10 cortical subregions revealed that a Shank2/3 deletion within the retrosplenial area severely impairs social memory, a core symptom of ASD. Notably, DREADD-mediated neuronal activation could rescue the social impairment triggered by Shank2/3 depletion. Data indicate that the retrosplenial area has to be added to the list of defined brain regions that contribute to the spectrum of behavioural alterations seen in ASDs.

Topics & Concepts

Retrosplenial cortexAutismNeuroscienceAutism spectrum disorderPsychologyKnockout mouseMedicinePsychiatryCortex (anatomy)ReceptorInternal medicineAutism Spectrum Disorder ResearchGenetics and Neurodevelopmental DisordersAttention Deficit Hyperactivity Disorder