Novel Genetic Variants of Sporadic Atrial Septal Defect (ASD) in a Chinese Population Identified by Whole-Exome Sequencing (WES)

BACKGROUND Recently, mutations in several genes have been described to be associated with sporadic ASD, but some genetic variants remain to be identified. The aim of this study was to use whole-exome sequencing (WES) combined with bioinformatics analysis to identify novel genetic variants in cases o...

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Published inMedical science monitor Vol. 24; pp. 1340 - 1358
Main Authors Liu, Yong, Cao, Yu, Li, Yaxiong, Lei, Dongyun, Li, Lin, Hou, Zong Liu, Han, Shen, Meng, Mingyao, Shi, Jianlin, Zhang, Yayong, Wang, Yi, Niu, Zhaoyi, Xie, Yanhua, Xiao, Benshan, Wang, Yuanfei, Li, Xiao, Yang, Lirong, Wang, Wenju, Jiang, Lihong
Format Journal Article
LanguageEnglish
Published United States International Scientific Literature, Inc 05.03.2018
Subjects
Adult
Asian Continental Ancestry Group - genetics
Cardiac Myosins - genetics
Cardiac Myosins - metabolism
China
Clinical Research
Computational Biology - methods
Exome
Exons
Female
Forkhead Box Protein L2 - genetics
Forkhead Box Protein L2 - metabolism
Genetic Predisposition to Disease
Genetic Variation
Heart Septal Defects, Atrial - genetics
Humans
Male
Microfilament Proteins - genetics
Microfilament Proteins - metabolism
Middle Aged
Mutation
Myosin Heavy Chains - genetics
Myosin Heavy Chains - metabolism
Sequence Analysis, DNA - methods
Whole Exome Sequencing - methods
Online AccessGet full text
ISSN1643-3750
1234-1010
1643-3750
DOI10.12659/MSM.908923

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Abstract BACKGROUND Recently, mutations in several genes have been described to be associated with sporadic ASD, but some genetic variants remain to be identified. The aim of this study was to use whole-exome sequencing (WES) combined with bioinformatics analysis to identify novel genetic variants in cases of sporadic congenital ASD, followed by validation by Sanger sequencing. MATERIAL AND METHODS Five Han patients with secundum ASD were recruited, and their tissue samples were analyzed by WES, followed by verification by Sanger sequencing of tissue and blood samples. Further evaluation using blood samples included 452 additional patients with sporadic secundum ASD (212 male and 240 female patients) and 519 healthy subjects (252 male and 267 female subjects) for further verification by a multiplexed MassARRAY system. Bioinformatic analyses were performed to identify novel genetic variants associated with sporadic ASD. RESULTS From five patients with sporadic ASD, a total of 181,762 genomic variants in 33 exon loci, validated by Sanger sequencing, were selected and underwent MassARRAY analysis in 452 patients with ASD and 519 healthy subjects. Three loci with high mutation frequencies, the 138665410 FOXL2 gene variant, the 23862952 MYH6 gene variant, and the 71098693 HYDIN gene variant were found to be significantly associated with sporadic ASD (P<0.05); variants in FOXL2 and MYH6 were found in patients with isolated, sporadic ASD (P<5×10^-4). CONCLUSIONS This was the first study that demonstrated variants in FOXL2 and HYDIN associated with sporadic ASD, and supported the use of WES and bioinformatics analysis to identify disease-associated mutations.
AbstractList BACKGROUND Recently, mutations in several genes have been described to be associated with sporadic ASD, but some genetic variants remain to be identified. The aim of this study was to use whole-exome sequencing (WES) combined with bioinformatics analysis to identify novel genetic variants in cases of sporadic congenital ASD, followed by validation by Sanger sequencing. MATERIAL AND METHODS Five Han patients with secundum ASD were recruited, and their tissue samples were analyzed by WES, followed by verification by Sanger sequencing of tissue and blood samples. Further evaluation using blood samples included 452 additional patients with sporadic secundum ASD (212 male and 240 female patients) and 519 healthy subjects (252 male and 267 female subjects) for further verification by a multiplexed MassARRAY system. Bioinformatic analyses were performed to identify novel genetic variants associated with sporadic ASD. RESULTS From five patients with sporadic ASD, a total of 181,762 genomic variants in 33 exon loci, validated by Sanger sequencing, were selected and underwent MassARRAY analysis in 452 patients with ASD and 519 healthy subjects. Three loci with high mutation frequencies, the 138665410 FOXL2 gene variant, the 23862952 MYH6 gene variant, and the 71098693 HYDIN gene variant were found to be significantly associated with sporadic ASD (P<0.05); variants in FOXL2 and MYH6 were found in patients with isolated, sporadic ASD (P<5×10^-4). CONCLUSIONS This was the first study that demonstrated variants in FOXL2 and HYDIN associated with sporadic ASD, and supported the use of WES and bioinformatics analysis to identify disease-associated mutations.BACKGROUND Recently, mutations in several genes have been described to be associated with sporadic ASD, but some genetic variants remain to be identified. The aim of this study was to use whole-exome sequencing (WES) combined with bioinformatics analysis to identify novel genetic variants in cases of sporadic congenital ASD, followed by validation by Sanger sequencing. MATERIAL AND METHODS Five Han patients with secundum ASD were recruited, and their tissue samples were analyzed by WES, followed by verification by Sanger sequencing of tissue and blood samples. Further evaluation using blood samples included 452 additional patients with sporadic secundum ASD (212 male and 240 female patients) and 519 healthy subjects (252 male and 267 female subjects) for further verification by a multiplexed MassARRAY system. Bioinformatic analyses were performed to identify novel genetic variants associated with sporadic ASD. RESULTS From five patients with sporadic ASD, a total of 181,762 genomic variants in 33 exon loci, validated by Sanger sequencing, were selected and underwent MassARRAY analysis in 452 patients with ASD and 519 healthy subjects. Three loci with high mutation frequencies, the 138665410 FOXL2 gene variant, the 23862952 MYH6 gene variant, and the 71098693 HYDIN gene variant were found to be significantly associated with sporadic ASD (P<0.05); variants in FOXL2 and MYH6 were found in patients with isolated, sporadic ASD (P<5×10^-4). CONCLUSIONS This was the first study that demonstrated variants in FOXL2 and HYDIN associated with sporadic ASD, and supported the use of WES and bioinformatics analysis to identify disease-associated mutations.
BACKGROUND Recently, mutations in several genes have been described to be associated with sporadic ASD, but some genetic variants remain to be identified. The aim of this study was to use whole-exome sequencing (WES) combined with bioinformatics analysis to identify novel genetic variants in cases of sporadic congenital ASD, followed by validation by Sanger sequencing. MATERIAL AND METHODS Five Han patients with secundum ASD were recruited, and their tissue samples were analyzed by WES, followed by verification by Sanger sequencing of tissue and blood samples. Further evaluation using blood samples included 452 additional patients with sporadic secundum ASD (212 male and 240 female patients) and 519 healthy subjects (252 male and 267 female subjects) for further verification by a multiplexed MassARRAY system. Bioinformatic analyses were performed to identify novel genetic variants associated with sporadic ASD. RESULTS From five patients with sporadic ASD, a total of 181,762 genomic variants in 33 exon loci, validated by Sanger sequencing, were selected and underwent MassARRAY analysis in 452 patients with ASD and 519 healthy subjects. Three loci with high mutation frequencies, the 138665410 FOXL2 gene variant, the 23862952 MYH6 gene variant, and the 71098693 HYDIN gene variant were found to be significantly associated with sporadic ASD (P<0.05); variants in FOXL2 and MYH6 were found in patients with isolated, sporadic ASD (P<5×10^-4). CONCLUSIONS This was the first study that demonstrated variants in FOXL2 and HYDIN associated with sporadic ASD, and supported the use of WES and bioinformatics analysis to identify disease-associated mutations.
Author Wang, Wenju
Li, Lin
Yang, Lirong
Wang, Yuanfei
Hou, Zong Liu
Meng, Mingyao
Shi, Jianlin
Wang, Yi
Niu, Zhaoyi
Xiao, Benshan
Zhang, Yayong
Jiang, Lihong
Li, Yaxiong
Xie, Yanhua
Cao, Yu
Han, Shen
Li, Xiao
Lei, Dongyun
Liu, Yong
AuthorAffiliation 1 Department of Cardiovascular Surgery, Yan’an Affiliated Hospital of Kunming Medical University, Kunming, Yunnan, P.R. China
2 Department of Cardiovascular Surgery, The First Peoples’ Hospital of Yunnan Province, Kunming, Yunnan, P.R. China
4 The First Affiliated Hospital of Kunming Medical University, Kunming, Yunnan, P.R. China
3 Key Laboratory of Cardiovascular Disease of Yunnan Province, Kunming, Yunnan, P.R. China
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  surname: Cao
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  givenname: Jianlin
  surname: Shi
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– sequence: 10
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  givenname: Zhaoyi
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– sequence: 13
  givenname: Yanhua
  surname: Xie
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  givenname: Benshan
  surname: Xiao
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  givenname: Yuanfei
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  surname: Jiang
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  organization: Department of Cardiovascular Surgery, The First Peoples’ Hospital of Yunnan Province, Kunming, Yunnan, China (mainland)
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Joint first authors; Yong Liu, Yu Cao, Yaxiong Li, Dongyun Lei
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Snippet BACKGROUND Recently, mutations in several genes have been described to be associated with sporadic ASD, but some genetic variants remain to be identified. The...
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SubjectTerms Adult
Asian Continental Ancestry Group - genetics
Cardiac Myosins - genetics
Cardiac Myosins - metabolism
China
Clinical Research
Computational Biology - methods
Exome
Exons
Female
Forkhead Box Protein L2 - genetics
Forkhead Box Protein L2 - metabolism
Genetic Predisposition to Disease
Genetic Variation
Heart Septal Defects, Atrial - genetics
Humans
Male
Microfilament Proteins - genetics
Microfilament Proteins - metabolism
Middle Aged
Mutation
Myosin Heavy Chains - genetics
Myosin Heavy Chains - metabolism
Sequence Analysis, DNA - methods
Whole Exome Sequencing - methods
Title Novel Genetic Variants of Sporadic Atrial Septal Defect (ASD) in a Chinese Population Identified by Whole-Exome Sequencing (WES)
URI https://www.ncbi.nlm.nih.gov/pubmed/29505555
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Volume 24
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