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Chromatin remodelling subunit SMARCB1 is implicated in dendrite development and complex brain functions

Created on 31 Oct 2025

Authors

Lemke, K. I., Filatova, A., Chiang, J., North, H., Kamphof, M. R. M., Becker-Roeck, M., Laube, B., Santen, G., Swaab, H., Nuber, U. A.

Abstract

SMARCB1 encodes a core component of the BAF chromatin remodelling complex and pathogenic variants in this gene are associated with neurodevelopmental disorders such as Coffin-Siris syndrome. The relationship between altered SMARCB1 protein products and severe functional brain changes in Coffin-Siris syndrome remains largely unknown. We performed cellular, molecular, and behavioural analyses of a Coffin-Siris syndrome mouse model with a heterozygous nervous system-specific Smarcb1 mutation. In addition, we evaluated general cognitive abilities, as well as cognitive and behavioural functioning, in individuals with SMARCB1-related Coffin-Siris syndrome. Smarcb1 mutant mice exhibited deficits in fine motor coordination and balance, as well as impaired spatial learning and memory. Furthermore, these mice showed anxiety-like behaviours and agitation when exposed to novel environments. The detected behavioural abnormalities could indicate impaired decision-making, which results in impaired risk assessment. Comparable cognitive and behavioural deviations were identified in individuals with Coffin-Siris syndrome and SMARCB1 pathogenic variants. Our analysis of the Smarcb1 mouse model revealed structural alterations in the brain, including decreased dendritic length and complexity of dendritic trees. These alterations may explain the observed functional impairments. Notably, our finding of reduced Wasl transcripts in mutant Purkinje cell nuclei suggests that dysregulation of actin polymerization may be involved in the discovered dendritic defects. Taken together, we demonstrate a link between the chromatin remodelling complex component SMARCB1, complex brain functions, neuronal structure, and a key regulator of actin branching.

Preprint server: bioRxiv
The authors list and abstract were imported from bioRxiv on 31 Oct 2025.

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