Identification of microduplications at Xp21.2 and Xq13.1 in neurodevelopmental disorders

Hannaleena Kokkonen; Auli Siren; Tuomo Määttä; Magda Kamila Kadlubowska; Anushree Acharya; Liz M. Nouel‐Saied; Suzanne M. Leal; Irma Järvelä; Isabelle Schrauwen

doi:10.1002/mgg3.1703

Molecular Genetics & Genomic Medicine (Dec 2021)

Identification of microduplications at Xp21.2 and Xq13.1 in neurodevelopmental disorders

Hannaleena Kokkonen,
Auli Siren,
Tuomo Määttä,
Magda Kamila Kadlubowska,
Anushree Acharya,
Liz M. Nouel‐Saied,
Suzanne M. Leal,
Irma Järvelä,
Isabelle Schrauwen

Affiliations

Hannaleena Kokkonen: Northern Finland Laboratory Centre NordLab and Medical Research Centre Oulu University Hospital and University of Oulu Oulu Finland
Auli Siren: Kanta‐Häme Central Hospital Hämeenlinna Finland
Tuomo Määttä: Disability Services Joint Authority for Kainuu Kajaani Finland
Magda Kamila Kadlubowska: Center for Statistical Genetics Sergievsky Center Department of Neurology Columbia University Medical Center New York NY USA
Anushree Acharya: Center for Statistical Genetics Sergievsky Center Department of Neurology Columbia University Medical Center New York NY USA
Liz M. Nouel‐Saied: Center for Statistical Genetics Sergievsky Center Department of Neurology Columbia University Medical Center New York NY USA
Suzanne M. Leal: Center for Statistical Genetics Sergievsky Center Department of Neurology Columbia University Medical Center New York NY USA
Irma Järvelä: Department of Medical Genetics University of Helsinki Helsinki Finland
Isabelle Schrauwen: Center for Statistical Genetics Sergievsky Center Department of Neurology Columbia University Medical Center New York NY USA

DOI: https://doi.org/10.1002/mgg3.1703
Journal volume & issue: Vol. 9, no. 12
pp. n/a – n/a

Abstract

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Abstract Background Microduplications are a rare cause of disease in X‐linked neurodevelopmental disorders but likely have been under reported due challenges in detection and interpretation. Methods We performed exome sequencing and subsequent microarray analysis in two families with a neurodevelopmental disorder. Results Here, we report on two families each with unique inherited microduplications at Xp21.2 and Xq13.1, respectively. In the first family, a 562.8‐kb duplication at Xq13.1 covering DLG3, TEX11, SLC7A3, GDPD2, and part KIF4A was identified in a boy whose phenotype was characterized by delayed speech development, mild intellectual disability (ID), mild dysmorphic facial features, a heart defect, and neuropsychiatric symptoms. By interrogating all reported Xq13.1 duplications in individuals affected with a neurodevelopmental disorder, we provide evidence that this genomic region and particularly DLG3 might be sensitive to an increased dosage. In the second family with four affected males, we found a noncontinuous 223‐ and 204‐kb duplication at Xp21.2, of which the first duplication covers exon 6 of IL1RAPL1. The phenotype of the male patients was characterized by delayed speech development, mild to moderate ID, strabismus, and neurobehavioral symptoms. The carrier daughter and her mother had learning difficulties. IL1RAPL1 shows nonrecurrent causal structural variation and is located at a common fragile site (FRAXC), prone to re‐arrangement. Conclusion In conclusion, we show that comprehensive clinical and genetic examination of microduplications on the X‐chromosome can be helpful in undiagnosed cases of neurodevelopmental disease.

Published in Molecular Genetics & Genomic Medicine

ISSN: 2324-9269 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/23249269

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