Journal article

SETBP1 variants outside the degron disrupt DNA-binding, transcription and neuronal differentiation capacity to cause a heterogeneous neurodevelopmental disorder

MMK Wong, RA Kampen, RO Braden, G Alagöz, MS Hildebrand, AJM Dingemans, J Corbally, J den Hoed, E Mendoza, WJJ Claassen, C Barnett, M Barnett, A Brusco, D Carli, BBA de Vries, F Elmslie, GB Ferrero, NA Jansen, IMBH van de Laar, A Moroni Show all

Nature Communications | Springer Science and Business Media LLC | Published : 2025

DOI: 10.1038/s41467-025-64074-x

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Abstract

Different types of germline de novo SETBP1 variants cause clinically distinct and heterogeneous neurodevelopmental disorders: Schinzel-Giedion syndrome (SGS, via missense variants at a critical degron region) and SETBP1-haploinsufficiency disorder. However, due to the lack of systematic investigation of genotype-phenotype associations of different types of SETBP1 variants, and limited understanding of its roles in neurodevelopment, the extent of clinical heterogeneity and how this relates to underlying pathophysiological mechanisms remains elusive. This imposes challenges for diagnosis. Here, we present a comprehensive investigation of the largest cohort to date of individuals carrying SETBP..

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Keywords

Genetics
2.1 Biological and Endogenous Factors
Intellectual and Developmental Disabilities (idd)
32 Biomedical and Clinical Sciences
Brain Disorders
3105 Genetics
Mental Health
Pediatric Research Initiative
Rare Diseases
1.1 Normal Biological Development and Functioning
Clinical Research
Neurosciences
31 Biological Sciences