De novo variants in MED12 cause X-linked syndromic neurodevelopmental disorders in 18 females
Polla DL, Bhoj EJ, Verheij JB, Wassink-Ruiter JS, Reis A, Deshpande C, Gregor A, Hill-Karfe K, Silfhout ATv, Pfundt R, Bongers EM, Hakonarson H, Berland S, Gradek G, Banka S, Chandler K, Gompertz L, Huffels SC, Stumpel CT, Wennekes R, Stegmann AP, Reardon W, Leenders EK, de Vries BB, Li D, Zackai E, Ragge N, Lynch SA, Cuddapah S, van Bokhoven H, Zweier C, de Brouwer AP (2020)
Publication Type: Journal article
Publication year: 2020
Journal
DOI: 10.1038/s41436-020-01040-6
Abstract
Purpose: MED12 is a subunit of the Mediator multiprotein complex with a central role in RNA polymerase II transcription and regulation of cell growth, development, and differentiation. This might underlie the variable phenotypes in males carrying missense variants in MED12, including X-linked recessive Ohdo, Lujan, and FG syndromes. Methods: By international matchmaking we assembled variant and clinical data on 18 females presenting with variable neurodevelopmental disorders (NDDs) and harboring de novo variants in MED12. Results: Five nonsense variants clustered in the C-terminal region, two splice variants were found in the same exon 8 splice acceptor site, and 11 missense variants were distributed over the gene/protein. Protein truncating variants were associated with a severe, syndromic phenotype consisting of intellectual disability (ID), facial dysmorphism, short stature, skeletal abnormalities, feeding difficulties, and variable other abnormalities. De novo missense variants were associated with a less specific, but homogeneous phenotype including severe ID, autistic features, limited speech and variable other anomalies, overlapping both with females with truncating variants as well as males with missense variants. Conclusion: We establish de novo truncating variants in MED12 as causative for a distinct NDD and de novo missense variants as causative for a severe, less specific NDD in females.
Authors with CRIS profile
André Wiesmann da Silva Reis
Lehrstuhl für Humangenetik
Anne Gregor
Institute of Human Genetics
Christiane Zweier
Medizinische Fakultät
Involved external institutions
Radboud University Nijmegen Medical Centre / Radboudumc of voluit Radboud Universitair Medisch Centrum (UMC)
Netherlands (NL)
Children's Hospital of Philadelphia
United States (USA) (US)
University of Groningen / Rijksuniversiteit Groningen
Netherlands (NL)
Guy's and St Thomas' (NHS Foundation Trust)
United Kingdom (GB)
Haukeland University Hospital / Haukeland universitetssykehus
Norway (NO)
University of Manchester
United Kingdom (GB)
Maastricht University
Netherlands (NL)
London School of Hygiene and Tropical Medicine
United Kingdom (GB)
University College Dublin (UCD)
Ireland (IE)
Netherlands (NL)
Children's Hospital of Philadelphia
United States (USA) (US)
University of Groningen / Rijksuniversiteit Groningen
Netherlands (NL)
Guy's and St Thomas' (NHS Foundation Trust)
United Kingdom (GB)
Haukeland University Hospital / Haukeland universitetssykehus
Norway (NO)
University of Manchester
United Kingdom (GB)
Maastricht University
Netherlands (NL)
London School of Hygiene and Tropical Medicine
United Kingdom (GB)
University College Dublin (UCD)
Ireland (IE)
How to cite
APA:
Polla, D.L., Bhoj, E.J., Verheij, J.B., Wassink-Ruiter, J.S., Reis, A., Deshpande, C.,... de Brouwer, A.P. (2020). De novo variants in MED12 cause X-linked syndromic neurodevelopmental disorders in 18 females. Genetics in Medicine. https://doi.org/10.1038/s41436-020-01040-6
MLA:
Polla, D. L., et al. "De novo variants in MED12 cause X-linked syndromic neurodevelopmental disorders in 18 females." Genetics in Medicine (2020).
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