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Protein destabilization underlies pathogenic missense mutations in ARID1B.

Fanny Mermet-MeillonSamuele MercanBeatrice Bauer-ProbstCyril AllardMelusine BleuKeith CalkinsJudith KnehrMarc AltorferUlrike NaumannKathleen SprouffskeLouise BarysFabian SesterhennGiorgio Giacomo Galli
Published in: Nature structural & molecular biology (2024)
ARID1B is a SWI/SNF subunit frequently mutated in human Coffin-Siris syndrome (CSS) and it is necessary for proliferation of ARID1A mutant cancers. While most CSS ARID1B aberrations introduce frameshifts or stop codons, the functional consequence of missense mutations found in ARID1B is unclear. We here perform saturated mutagenesis screens on ARID1B and demonstrate that protein destabilization is the main mechanism associated with pathogenic missense mutations in patients with Coffin-Siris Syndrome.
Keyphrases
  • intellectual disability
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  • protein protein
  • gene expression
  • autism spectrum disorder
  • copy number
  • induced pluripotent stem cells