De Novo Mutations Affecting the Catalytic Cα Subunit of PP2A, PPP2CA, Cause Syndromic Intellectual Disability Resembling Other PP2A-Related Neurodevelopmental Disorders
Reynhout, Sara; Jansen, Sandra; Haesen, Dorien; van Belle, Siska; de Munnik, Sonja A.; Bongers, Ernie M.H.F.; Schieving, Jolanda H.; Marcelis, Carlo; Amiel, Jeanne; Rio, Marlène; Mclaughlin, Heather; Ladda, Roger; Sell, Susan; Kriek, Marjolein; Peeters-Scholte, Cacha M.P.C.D.; Terhal, Paulien A.; van Gassen, Koen L.; Verbeek, Nienke; Henry, Sonja; Scott Schwoerer, Jessica; Malik, Saleem; Revencu, Nicole; Ferreira, Carlos R.; Macnamara, Ellen; Braakman, Hilde M.H.; Brimble, Elise; Ruznikov, Maura R.Z.; Wagner, Matias; Harrer, Philip; Wieczorek, Dagmar; Kuechler, Alma; Tziperman, Barak; Barel, Ortal; de Vries, Bert B.A.; Gordon, Christopher T.; Janssens, Veerle; Vissers, Lisenka E.L.M.
(2019) American Journal of Human Genetics, volume 104, issue 1, pp. 139 - 156
(Article)
Abstract
Type 2A protein phosphatases (PP2As) are highly expressed in the brain and regulate neuronal signaling by catalyzing phospho-Ser/Thr dephosphorylations in diverse substrates. PP2A holoenzymes comprise catalytic C-, scaffolding A-, and regulatory B-type subunits, which determine substrate specificity and physiological function. Interestingly, de novo mutations in genes encoding A- and B-type
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subunits have recently been implicated in intellectual disability (ID) and developmental delay (DD). We now report 16 individuals with mild to profound ID and DD and a de novo mutation in PPP2CA, encoding the catalytic Cα subunit. Other frequently observed features were severe language delay (71%), hypotonia (69%), epilepsy (63%), and brain abnormalities such as ventriculomegaly and a small corpus callosum (67%). Behavioral problems, including autism spectrum disorders, were reported in 47% of individuals, and three individuals had a congenital heart defect. PPP2CA de novo mutations included a partial gene deletion, a frameshift, three nonsense mutations, a single amino acid duplication, a recurrent mutation, and eight non-recurrent missense mutations. Functional studies showed complete PP2A dysfunction in four individuals with seemingly milder ID, hinting at haploinsufficiency. Ten other individuals showed mutation-specific biochemical distortions, including poor expression, altered binding to the A subunit and specific B-type subunits, and impaired phosphatase activity and C-terminal methylation. Four were suspected to have a dominant-negative mechanism, which correlated with severe ID. Two missense variants affecting the same residue largely behaved as wild-type in our functional assays. Overall, we found that pathogenic PPP2CA variants impair PP2A-B56(δ) functionality, suggesting that PP2A-related neurodevelopmental disorders constitute functionally converging ID syndromes.
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Keywords: de novo mutation, epilepsy, intellectual disability, PP2A, PP2A-related neurodevelopmental disorders, PPP2CA, syndrome, Genetics, Genetics(clinical)
ISSN: 0002-9297
Publisher: Cell Press
Note: Funding Information: The authors thank the individuals and their parents for participating in the study. Funding was provided by the IAP program of the Belgian federal government (P7/13 to V.J.), Research Foundation-Flanders (to V.J.), and the University of Leuven (C24/17/073 to V.J.). S.R. received an FWO-SB fellowship from the Research Foundation-Flanders. D.H. received a fellowship of the Flemish Agency for Innovation by Science and Technology. This work was financially supported by grants from the Netherlands Organization for Health Research and Development (917-86-319 and 912-12-109 to B.B.A.d.V.) and made use of data generated by the DECIPHER Consortium. A full list of centers who contributed to the generation of the data is available at https://decipher.sanger.ac.uk/ and via email at decipher@sanger.ac.uk. Funding for the project was provided by the Wellcome Trust. Funding Information: The authors thank the individuals and their parents for participating in the study. Funding was provided by the IAP program of the Belgian federal government ( P7/13 to V.J.), Research Foundation-Flanders (to V.J.), and the University of Leuven ( C24/17/073 to V.J.). S.R. received an FWO-SB fellowship from the Research Foundation-Flanders . D.H. received a fellowship of the Flemish Agency for Innovation by Science and Technology . This work was financially supported by grants from the Netherlands Organization for Health Research and Development ( 917-86-319 and 912-12-109 to B.B.A.d.V.) and made use of data generated by the DECIPHER Consortium. A full list of centers who contributed to the generation of the data is available at https://decipher.sanger.ac.uk/ and via email at decipher@sanger.ac.uk . Funding for the project was provided by the Wellcome Trust . Publisher Copyright: © 2018 American Society of Human Genetics
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