BACKGROUND: We present a large Dutch family with seven males affected by a novel syndrome of X-linked intellectual disability, hypogonadism, gynaecomastia, truncal obesity, short stature and recognisable craniofacial manifestations resembling but not identical to Wilson-Turner syndrome. Seven female relatives show a much milder expression of the phenotype. METHODS AND RESULTS: We performed X chromosome exome (X-exome) sequencing in five individuals from this family and identified a novel intronic variant in the histone deacetylase 8 gene (HDAC8), c.164+5G>A, which disturbs the normal splicing of exon 2 resulting in exon skipping, and introduces a premature stop at the beginning of the histone deacetylase catalytic domain. The identified variant completely segregates in this family and was absent in 96 Dutch controls and available databases. Affected female carriers showed a notably skewed X-inactivation pattern in lymphocytes in which the mutated X-chromosome was completely inactivated. CONCLUSIONS: HDAC8 is a member of the protein family of histone deacetylases that play a major role in epigenetic gene silencing during development. HDAC8 specifically controls the patterning of the skull with the mouse HDAC8 knock-out showing craniofacial deformities of the skull. The present family provides the first evidence for involvement of HDAC8 in a syndromic form of intellectual disability.
BACKGROUND: We present a large Dutch family with seven males affected by a novel syndrome of X-linked intellectual disability, hypogonadism, gynaecomastia, truncal obesity, short stature and recognisable craniofacial manifestations resembling but not identical to Wilson-Turner syndrome. Seven female relatives show a much milder expression of the phenotype. METHODS AND RESULTS: We performed X chromosome exome (X-exome) sequencing in five individuals from this family and identified a novel intronic variant in the histone deacetylase 8 gene (HDAC8), c.164+5G>A, which disturbs the normal splicing of exon 2 resulting in exon skipping, and introduces a premature stop at the beginning of the histone deacetylase catalytic domain. The identified variant completely segregates in this family and was absent in 96 Dutch controls and available databases. Affected female carriers showed a notably skewed X-inactivation pattern in lymphocytes in which the mutated X-chromosome was completely inactivated. CONCLUSIONS:HDAC8 is a member of the protein family of histone deacetylases that play a major role in epigenetic gene silencing during development. HDAC8 specifically controls the patterning of the skull with the mouseHDAC8 knock-out showing craniofacial deformities of the skull. The present family provides the first evidence for involvement of HDAC8 in a syndromic form of intellectual disability.
Authors: Elizabeth W Bradley; Lomeli R Carpio; Andre J van Wijnen; Meghan E McGee-Lawrence; Jennifer J Westendorf Journal: Physiol Rev Date: 2015-10 Impact factor: 37.312
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Authors: Frank J Kaiser; Morad Ansari; Diana Braunholz; María Concepción Gil-Rodríguez; Christophe Decroos; Jonathan J Wilde; Christopher T Fincher; Maninder Kaur; Masashige Bando; David J Amor; Paldeep S Atwal; Melanie Bahlo; Christine M Bowman; Jacquelyn J Bradley; Han G Brunner; Dinah Clark; Miguel Del Campo; Nataliya Di Donato; Peter Diakumis; Holly Dubbs; David A Dyment; Juliane Eckhold; Sarah Ernst; Jose C Ferreira; Lauren J Francey; Ulrike Gehlken; Encarna Guillén-Navarro; Yolanda Gyftodimou; Bryan D Hall; Raoul Hennekam; Louanne Hudgins; Melanie Hullings; Jennifer M Hunter; Helger Yntema; A Micheil Innes; Antonie D Kline; Zita Krumina; Hane Lee; Kathleen Leppig; Sally Ann Lynch; Mark B Mallozzi; Linda Mannini; Shane McKee; Sarju G Mehta; Ieva Micule; Shehla Mohammed; Ellen Moran; Geert R Mortier; Joe-Ann S Moser; Sarah E Noon; Naohito Nozaki; Luis Nunes; John G Pappas; Lynette S Penney; Antonio Pérez-Aytés; Michael B Petersen; Beatriz Puisac; Nicole Revencu; Elizabeth Roeder; Sulagna Saitta; Angela E Scheuerle; Karen L Schindeler; Victoria M Siu; Zornitza Stark; Samuel P Strom; Heidi Thiese; Inga Vater; Patrick Willems; Kathleen Williamson; Louise C Wilson; Hakon Hakonarson; Fabiola Quintero-Rivera; Jolanta Wierzba; Antonio Musio; Gabriele Gillessen-Kaesbach; Feliciano J Ramos; Laird G Jackson; Katsuhiko Shirahige; Juan Pié; David W Christianson; Ian D Krantz; David R Fitzpatrick; Matthew A Deardorff Journal: Hum Mol Genet Date: 2014-01-08 Impact factor: 5.121