Paroxysmal Movement Disorder and Epilepsy Caused by a De Novo Truncating Mutation in KAT6A
Stephanie Efthymiou
1
Department of Molecular Neuroscience, Institute of Neurology, University College London, London, United Kingdom
2
Department of Clinical and Experimental Epilepsy, Institute of Neurology, University College London, London, United Kingdom
,
Vincenzo Salpietro
1
Department of Molecular Neuroscience, Institute of Neurology, University College London, London, United Kingdom
,
Conceicao Bettencourt
1
Department of Molecular Neuroscience, Institute of Neurology, University College London, London, United Kingdom
2
Department of Clinical and Experimental Epilepsy, Institute of Neurology, University College London, London, United Kingdom
,
Henry Houlden
1
Department of Molecular Neuroscience, Institute of Neurology, University College London, London, United Kingdom
› Author AffiliationsFunding This study was supported in part by The Wellcome Trust in equipment and strategic award (Synaptopathies) funding (WT093205 MA and WT104033AIA).
Mutations in KAT6A encoding a histone acetyltransferase involved in chromatin remodeling and in other genes involved in histone acetylation and/or deacetylation have been implicated in broad phenotypes of congenital and developmental abnormalities. However, limited genotype–phenotype correlations are available for some of the most rare or recently reported genetic disorders related to chromatin dysregulation. We hereby report a de novo truncating mutation in KAT6A (c.3338C > G; p.S1113X) in a young male patient with intellectual disability associated with impaired speech and autistic features, who also presented with infantile seizures and a complex movement disorder phenotype with paroxysmal episodes of abnormal startle responses.
Keywords
KAT6A -
startle reflex syndrome -
global developmental delay
Ethical Publication Statement
We confirm that we have read the Journal's position on issues involved in ethical publication and affirm that this report is consistent with those guidelines.
Author Contributions
Stephanie Efthymiou: study design and experimental data acquisition, analysis and interpretation of data.
Dr. Vincenzo Salpietro: study concept and clinical data contribution to the manuscript, analysis and interpretation of data.
Dr. Conceicao Bettencourt: critical revision of the manuscript document.
Prof. Henry Houlden: study supervision.
References
1
Mencacci NE,
Kamsteeg EJ,
Nakashima K.
, et al. De novo mutations in PDE10A cause childhood-onset chorea with bilateral striatal lesions. Am J Hum Genet 2016; 98 (04) 763-771
2
Dreissen YEM,
Boeree T,
Koelman JHTM,
Tijssen MAJ.
Startle responses in functional jerky movement disorders are increased but have a normal pattern. Parkinsonism Relat Disord 2017; 40: 27-32
3
Tham E,
Lindstrand A,
Santani A.
, et al. Dominant mutations in KAT6A cause intellectual disability with recognizable syndromic features. Am J Hum Genet 2015; 96 (03) 507-513
5
Millan F,
Cho MT,
Retterer K.
, et al. Whole exome sequencing reveals de novo pathogenic variants in KAT6A as a cause of a neurodevelopmental disorder. Am J Med Genet A 2016; 170 (07) 1791-1798
6
Arboleda VA,
Lee H,
Dorrani N.
, et al; UCLA Clinical Genomics Center. De novo nonsense mutations in KAT6A, a lysine acetyl-transferase gene, cause a syndrome including microcephaly and global developmental delay. Am J Hum Genet 2015; 96 (03) 498-506
7
Zwaveling-Soonawala N,
Alders M,
Jongejan A.
, et al. Clues for polygenic inheritance of pituitary stalk interruption syndrome from exome sequencing in 20 patients. J Clin Endocrinol Metab 2018; 103 (02) 415-428
8
Good-Jacobson KL,
Chen Y,
Voss AK,
Smyth GK,
Thomas T,
Tarlinton D.
Regulation of germinal center responses and B-cell memory by the chromatin modifier MOZ. Proc Natl Acad Sci U S A 2014; 111 (26) 9585-9590
