CUL3-related neurodevelopmental disorder: Clinical phenotype of 20 new individuals and identification of a potential phenotype-associated episignature
Publication date
2025-01-09
Authors
van der Laan, Liselot
Silva, Ananília
Kleinendorst, Lotte
Rooney, Kathleen
Haghshenas, Sadegheh
Lauffer, Peter
Alanay, Yasemin
Bhai, Pratibha
Brusco, Alfredo
de Munnik, Sonja
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Advisors
Supervisors
Document Type
Article
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Abstract
Neurodevelopmental disorder with or without autism or seizures (NEDAUS) is a neurodevelopmental disorder characterized by global developmental delay, speech delay, seizures, autistic features, and/or behavior abnormalities. It is caused by CUL3 (Cullin-3 ubiquitin ligase) haploinsufficiency. We collected clinical and molecular data from 26 individuals carrying pathogenic variants and variants of uncertain significance (VUS) in the CUL3 gene, including 20 previously unreported cases. By comparing their DNA methylation (DNAm) classifiers with those of healthy controls and other neurodevelopmental disorders characterized by established episignatures, we aimed to create a diagnostic biomarker (episignature) and gain more knowledge of the molecular pathophysiology. We discovered a sensitive and specific DNAm episignature for patients with pathogenic variants in CUL3 and utilized it to reclassify patients carrying a VUS in the CUL3 gene. Comparative epigenomic analysis revealed similarities between NEDAUS and several other rare genetic neurodevelopmental disorders with previously identified episignatures, highlighting the broader implication of our findings. In addition, we performed genotype-phenotype correlation studies to explain the variety in clinical presentation between the cases. We discovered a highly accurate DNAm episignature serving as a robust diagnostic biomarker for NEDAUS. Furthermore, we broadened the phenotypic spectrum by identifying 20 new individuals and confirming five previously reported cases of NEDAUS.
Keywords
CUL3, DNA methylation, episignature, genotype-phenotype correlation, intellectual disability, NEDAUS, Molecular Medicine, Genetics(clinical)
Citation
van der Laan, L, Silva, A, Kleinendorst, L, Rooney, K, Haghshenas, S, Lauffer, P, Alanay, Y, Bhai, P, Brusco, A, de Munnik, S, de Vries, B B A, Vega, A D, Engelen, M, Hopman, S, Herkert, J C, Hochstenbach, R, Kant, S G, Kira, R, Kato, M, Keren, B, Kroes, H Y, Levy, M A, Lock-Hock, N, Maas, S M, Mancini, G M S, Marcelis, C, Matsumoto, N, Mizuguchi, T, Mussa, A, Mignot, C, Närhi, A, Nordgren, A, Pfundt, R, Polstra, A M, Trajkova, S, van Bever, Y, José van den Boogaard, M, van der Smagt, J J, Barakat, T S, Alders, M, Mannens, M M A M, Sadikovic, B, van Haelst, M M & Henneman, P 2025, 'CUL3-related neurodevelopmental disorder : Clinical phenotype of 20 new individuals and identification of a potential phenotype-associated episignature', Human Genetics and Genomics Advances, vol. 6, no. 1, 100380. https://doi.org/10.1016/j.xhgg.2024.100380