Gonadal mosaicism of large terminal de novo duplication and deletion in siblings with variable intellectual disability phenotypes

BACKGROUND: Intellectual disability (ID) is a complex condition that can impact multiple domains of development. The genetic contribution to ID’s etiology is significant, with more than 100 implicated genes and loci currently identified. The majority of such variants are rare and de novo genetic mut...

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Autores principales: Rahman, Muhammad M., Uddin, KM Furkan, Al Jezawi, Nesreen K., Karuvantevida, Noushad, Akter, Hosneara, Dity, Nushrat J., Rahaman, Md. Ashiquir, Begum, Maksuda, Rahaman, Md. Atikur, Baqui, Md. Abdul, Salwa, Zeena, Islam, Serajul, Woodbury‐Smith, Marc, Basiruzzaman, Mohammed, Uddin, Mohammed
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6785528/
https://www.ncbi.nlm.nih.gov/pubmed/31475484
http://dx.doi.org/10.1002/mgg3.954
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author Rahman, Muhammad M.
Uddin, KM Furkan
Al Jezawi, Nesreen K.
Karuvantevida, Noushad
Akter, Hosneara
Dity, Nushrat J.
Rahaman, Md. Ashiquir
Begum, Maksuda
Rahaman, Md. Atikur
Baqui, Md. Abdul
Salwa, Zeena
Islam, Serajul
Woodbury‐Smith, Marc
Basiruzzaman, Mohammed
Uddin, Mohammed
author_facet Rahman, Muhammad M.
Uddin, KM Furkan
Al Jezawi, Nesreen K.
Karuvantevida, Noushad
Akter, Hosneara
Dity, Nushrat J.
Rahaman, Md. Ashiquir
Begum, Maksuda
Rahaman, Md. Atikur
Baqui, Md. Abdul
Salwa, Zeena
Islam, Serajul
Woodbury‐Smith, Marc
Basiruzzaman, Mohammed
Uddin, Mohammed
author_sort Rahman, Muhammad M.
collection PubMed
description BACKGROUND: Intellectual disability (ID) is a complex condition that can impact multiple domains of development. The genetic contribution to ID’s etiology is significant, with more than 100 implicated genes and loci currently identified. The majority of such variants are rare and de novo genetic mutations. METHODS: We have applied whole‐genome microarray to identify large, rare, clinically relevant copy number variants (CNVs). We have applied well‐established algorithms for variants call. Quantitative polymerase chain reaction (qPCR) was applied to validate the variants using three technical replicates for each family member. To assess whether the copy number variation was due to balanced translocation or mosaicism, we further conducted droplet digital PCR (ddPCR) on the whole family. We have, as well, applied “critical‐exon” mapping, human developmental brain transcriptome, and a database of known associated neurodevelopmental disorder variants to identify candidate genes. RESULTS: Here we present two siblings who are both impacted by a large terminal duplication and a deletion. Whole‐genome microarray revealed an 18.82 megabase (MB) duplication at terminal locus (7q34‐q36.3) of chromosome 7 and a 3.90 MB deletion impacting the terminal locus (15q26.3) of chromosome 15. qPCR and ddPCR experiments confirmed the de novo origin of the variants and the co‐occurrence of these two de novo events among the siblings, but their absence in both parents, implicates an unbalanced translocation that could have mal‐segregated among the siblings or a possible germline mosaicism. These terminal events impact IGF1R, CNTNAP2, and DPP6, shown to be strongly associated with neurodevelopmental disorders. Detailed clinical examination of the siblings revealed the presence of both shared and distinct phenotypic features. CONCLUSIONS: This study identified two large rare terminal de novo events impacting two siblings. Further phenotypic investigation highlights that even in the presence of identical large high penetrant variants, spectrum of clinical features can be different between the siblings.
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spelling pubmed-67855282019-10-17 Gonadal mosaicism of large terminal de novo duplication and deletion in siblings with variable intellectual disability phenotypes Rahman, Muhammad M. Uddin, KM Furkan Al Jezawi, Nesreen K. Karuvantevida, Noushad Akter, Hosneara Dity, Nushrat J. Rahaman, Md. Ashiquir Begum, Maksuda Rahaman, Md. Atikur Baqui, Md. Abdul Salwa, Zeena Islam, Serajul Woodbury‐Smith, Marc Basiruzzaman, Mohammed Uddin, Mohammed Mol Genet Genomic Med Original Articles BACKGROUND: Intellectual disability (ID) is a complex condition that can impact multiple domains of development. The genetic contribution to ID’s etiology is significant, with more than 100 implicated genes and loci currently identified. The majority of such variants are rare and de novo genetic mutations. METHODS: We have applied whole‐genome microarray to identify large, rare, clinically relevant copy number variants (CNVs). We have applied well‐established algorithms for variants call. Quantitative polymerase chain reaction (qPCR) was applied to validate the variants using three technical replicates for each family member. To assess whether the copy number variation was due to balanced translocation or mosaicism, we further conducted droplet digital PCR (ddPCR) on the whole family. We have, as well, applied “critical‐exon” mapping, human developmental brain transcriptome, and a database of known associated neurodevelopmental disorder variants to identify candidate genes. RESULTS: Here we present two siblings who are both impacted by a large terminal duplication and a deletion. Whole‐genome microarray revealed an 18.82 megabase (MB) duplication at terminal locus (7q34‐q36.3) of chromosome 7 and a 3.90 MB deletion impacting the terminal locus (15q26.3) of chromosome 15. qPCR and ddPCR experiments confirmed the de novo origin of the variants and the co‐occurrence of these two de novo events among the siblings, but their absence in both parents, implicates an unbalanced translocation that could have mal‐segregated among the siblings or a possible germline mosaicism. These terminal events impact IGF1R, CNTNAP2, and DPP6, shown to be strongly associated with neurodevelopmental disorders. Detailed clinical examination of the siblings revealed the presence of both shared and distinct phenotypic features. CONCLUSIONS: This study identified two large rare terminal de novo events impacting two siblings. Further phenotypic investigation highlights that even in the presence of identical large high penetrant variants, spectrum of clinical features can be different between the siblings. John Wiley and Sons Inc. 2019-09-01 /pmc/articles/PMC6785528/ /pubmed/31475484 http://dx.doi.org/10.1002/mgg3.954 Text en © 2019 The Authors. Molecular Genetics & Genomic Medicine published by Wiley Periodicals, Inc. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Rahman, Muhammad M.
Uddin, KM Furkan
Al Jezawi, Nesreen K.
Karuvantevida, Noushad
Akter, Hosneara
Dity, Nushrat J.
Rahaman, Md. Ashiquir
Begum, Maksuda
Rahaman, Md. Atikur
Baqui, Md. Abdul
Salwa, Zeena
Islam, Serajul
Woodbury‐Smith, Marc
Basiruzzaman, Mohammed
Uddin, Mohammed
Gonadal mosaicism of large terminal de novo duplication and deletion in siblings with variable intellectual disability phenotypes
title Gonadal mosaicism of large terminal de novo duplication and deletion in siblings with variable intellectual disability phenotypes
title_full Gonadal mosaicism of large terminal de novo duplication and deletion in siblings with variable intellectual disability phenotypes
title_fullStr Gonadal mosaicism of large terminal de novo duplication and deletion in siblings with variable intellectual disability phenotypes
title_full_unstemmed Gonadal mosaicism of large terminal de novo duplication and deletion in siblings with variable intellectual disability phenotypes
title_short Gonadal mosaicism of large terminal de novo duplication and deletion in siblings with variable intellectual disability phenotypes
title_sort gonadal mosaicism of large terminal de novo duplication and deletion in siblings with variable intellectual disability phenotypes
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6785528/
https://www.ncbi.nlm.nih.gov/pubmed/31475484
http://dx.doi.org/10.1002/mgg3.954
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