Amplicon Resequencing Identified Parental Mosaicism for Approximately 10% of “de novo” SCN1A Mutations in Children with Dravet Syndrome

The majority of children with Dravet syndrome (DS) are caused by de novo SCN1A mutations. To investigate the origin of the mutations, we developed and applied a new method that combined deep amplicon resequencing with a Bayesian model to detect and quantify allelic fractions with improved sensitivit...

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Autores principales: Xu, Xiaojing, Yang, Xiaoxu, Wu, Qixi, Liu, Aijie, Yang, Xiaoling, Ye, Adam Yongxin, Huang, August Yue, Li, Jiarui, Wang, Meng, Yu, Zhe, Wang, Sheng, Zhang, Zhichao, Wu, Xiru, Wei, Liping, Zhang, Yuehua
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2015
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5034833/
https://www.ncbi.nlm.nih.gov/pubmed/26096185
http://dx.doi.org/10.1002/humu.22819
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author Xu, Xiaojing
Yang, Xiaoxu
Wu, Qixi
Liu, Aijie
Yang, Xiaoling
Ye, Adam Yongxin
Huang, August Yue
Li, Jiarui
Wang, Meng
Yu, Zhe
Wang, Sheng
Zhang, Zhichao
Wu, Xiru
Wei, Liping
Zhang, Yuehua
author_facet Xu, Xiaojing
Yang, Xiaoxu
Wu, Qixi
Liu, Aijie
Yang, Xiaoling
Ye, Adam Yongxin
Huang, August Yue
Li, Jiarui
Wang, Meng
Yu, Zhe
Wang, Sheng
Zhang, Zhichao
Wu, Xiru
Wei, Liping
Zhang, Yuehua
author_sort Xu, Xiaojing
collection PubMed
description The majority of children with Dravet syndrome (DS) are caused by de novo SCN1A mutations. To investigate the origin of the mutations, we developed and applied a new method that combined deep amplicon resequencing with a Bayesian model to detect and quantify allelic fractions with improved sensitivity. Of 174 SCN1A mutations in DS probands which were considered “de novo” by Sanger sequencing, we identified 15 cases (8.6%) of parental mosaicism. We identified another five cases of parental mosaicism that were also detectable by Sanger sequencing. Fraction of mutant alleles in the 20 cases of parental mosaicism ranged from 1.1% to 32.6%. Thirteen (65% of 20) mutations originated paternally and seven (35% of 20) maternally. Twelve (60% of 20) mosaic parents did not have any epileptic symptoms. Their mutant allelic fractions were significantly lower than those in mosaic parents with epileptic symptoms (P = 0.016). We identified mosaicism with varied allelic fractions in blood, saliva, urine, hair follicle, oral epithelium, and semen, demonstrating that postzygotic mutations could affect multiple somatic cells as well as germ cells. Our results suggest that more sensitive tools for detecting low‐level mosaicism in parents of families with seemingly “de novo” mutations will allow for better informed genetic counseling.
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spelling pubmed-50348332016-10-03 Amplicon Resequencing Identified Parental Mosaicism for Approximately 10% of “de novo” SCN1A Mutations in Children with Dravet Syndrome Xu, Xiaojing Yang, Xiaoxu Wu, Qixi Liu, Aijie Yang, Xiaoling Ye, Adam Yongxin Huang, August Yue Li, Jiarui Wang, Meng Yu, Zhe Wang, Sheng Zhang, Zhichao Wu, Xiru Wei, Liping Zhang, Yuehua Hum Mutat Research Articles The majority of children with Dravet syndrome (DS) are caused by de novo SCN1A mutations. To investigate the origin of the mutations, we developed and applied a new method that combined deep amplicon resequencing with a Bayesian model to detect and quantify allelic fractions with improved sensitivity. Of 174 SCN1A mutations in DS probands which were considered “de novo” by Sanger sequencing, we identified 15 cases (8.6%) of parental mosaicism. We identified another five cases of parental mosaicism that were also detectable by Sanger sequencing. Fraction of mutant alleles in the 20 cases of parental mosaicism ranged from 1.1% to 32.6%. Thirteen (65% of 20) mutations originated paternally and seven (35% of 20) maternally. Twelve (60% of 20) mosaic parents did not have any epileptic symptoms. Their mutant allelic fractions were significantly lower than those in mosaic parents with epileptic symptoms (P = 0.016). We identified mosaicism with varied allelic fractions in blood, saliva, urine, hair follicle, oral epithelium, and semen, demonstrating that postzygotic mutations could affect multiple somatic cells as well as germ cells. Our results suggest that more sensitive tools for detecting low‐level mosaicism in parents of families with seemingly “de novo” mutations will allow for better informed genetic counseling. John Wiley and Sons Inc. 2015-07-24 2015-09 /pmc/articles/PMC5034833/ /pubmed/26096185 http://dx.doi.org/10.1002/humu.22819 Text en © 2015 The Authors. **Human Mutation published by Wiley Periodicals, Inc. This is an open access article under the terms of the Creative Commons Attribution‐NonCommercial‐NoDerivs (http://creativecommons.org/licenses/by-nc-nd/4.0/) License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Research Articles
Xu, Xiaojing
Yang, Xiaoxu
Wu, Qixi
Liu, Aijie
Yang, Xiaoling
Ye, Adam Yongxin
Huang, August Yue
Li, Jiarui
Wang, Meng
Yu, Zhe
Wang, Sheng
Zhang, Zhichao
Wu, Xiru
Wei, Liping
Zhang, Yuehua
Amplicon Resequencing Identified Parental Mosaicism for Approximately 10% of “de novo” SCN1A Mutations in Children with Dravet Syndrome
title Amplicon Resequencing Identified Parental Mosaicism for Approximately 10% of “de novo” SCN1A Mutations in Children with Dravet Syndrome
title_full Amplicon Resequencing Identified Parental Mosaicism for Approximately 10% of “de novo” SCN1A Mutations in Children with Dravet Syndrome
title_fullStr Amplicon Resequencing Identified Parental Mosaicism for Approximately 10% of “de novo” SCN1A Mutations in Children with Dravet Syndrome
title_full_unstemmed Amplicon Resequencing Identified Parental Mosaicism for Approximately 10% of “de novo” SCN1A Mutations in Children with Dravet Syndrome
title_short Amplicon Resequencing Identified Parental Mosaicism for Approximately 10% of “de novo” SCN1A Mutations in Children with Dravet Syndrome
title_sort amplicon resequencing identified parental mosaicism for approximately 10% of “de novo” scn1a mutations in children with dravet syndrome
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5034833/
https://www.ncbi.nlm.nih.gov/pubmed/26096185
http://dx.doi.org/10.1002/humu.22819
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