Cargando…
Validation and Disease Risk Assessment of Previously Reported Genome-Wide Genetic Variants Associated With Brugada Syndrome: SADS-TW BrS Registry
BACKGROUND: Brugada syndrome (BrS) is an oligogenic arrhythmic disease with increased risk of sudden cardiac arrest. Several BrS or ECG traits-related single-nucleotide polymorphisms (SNPs) were identified through previous genome-wide association studies in white patients. We aimed to validate these...
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Lippincott Williams & Wilkins
2020
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7439932/ https://www.ncbi.nlm.nih.gov/pubmed/32490690 http://dx.doi.org/10.1161/CIRCGEN.119.002797 |
| _version_ | 1783573067287494656 |
|---|---|
| author | Jimmy Juang, Jyh-Ming Liu, Yen-Bin Julius Chen, Ching-Yu Yu, Qi-You Chattopadhyay, Amrita Lin, Lian-Yu Chen, Wen-Jone Yu, Chih-Chien Huang, Hui-Chun Ho, Li-Ting Lai, Ling-Ping Hwang, Juey-Jen Lin, Ting-Tse Liao, Min-Tsun Chen, Jien-Jiun Sherri Yeh, Shih-Fan Chuang, Jing-Yuan Yang, Dun-Hui Lin, Jiunn-Lee Lu, Tzu-Pin Chuang, Eric Y. Ackerman, Michael J. |
| author_facet | Jimmy Juang, Jyh-Ming Liu, Yen-Bin Julius Chen, Ching-Yu Yu, Qi-You Chattopadhyay, Amrita Lin, Lian-Yu Chen, Wen-Jone Yu, Chih-Chien Huang, Hui-Chun Ho, Li-Ting Lai, Ling-Ping Hwang, Juey-Jen Lin, Ting-Tse Liao, Min-Tsun Chen, Jien-Jiun Sherri Yeh, Shih-Fan Chuang, Jing-Yuan Yang, Dun-Hui Lin, Jiunn-Lee Lu, Tzu-Pin Chuang, Eric Y. Ackerman, Michael J. |
| author_sort | Jimmy Juang, Jyh-Ming |
| collection | PubMed |
| description | BACKGROUND: Brugada syndrome (BrS) is an oligogenic arrhythmic disease with increased risk of sudden cardiac arrest. Several BrS or ECG traits-related single-nucleotide polymorphisms (SNPs) were identified through previous genome-wide association studies in white patients. We aimed to validate these SNPs in BrS patients in the Taiwanese population, assessing the cumulative effect of risk alleles and the BrS-polygenic risk score in predicting cardiac events. METHODS: We genotyped 190 unrelated BrS patients using the TWB Array, and Taiwan Biobank was used as controls. SNPs not included in the array were imputed by IMPUTE2. Cox proportional hazards model was used to evaluate the associations between each particular SNP, the collective BrS-polygenic risk score, and clinical outcomes. RESULTS: Of the 88 previously reported SNPs, 22 were validated in Taiwanese BrS patients (P<0.05). Of the 22 SNPs, 2 (rs10428132 and rs9388451) were linked with susceptibility to BrS, 10 were SNPs previously reaching genome-wide significance, and 10 were SNPs associated with ECG traits. For the 3 most commonly reported SNPs, disease risk increased consistently with the number of risk alleles (odds ratio, 3.54; P(trend)=1.38×10(−9) for 5 risk alleles versus 1). Similar patterns were observed in both SCN5A mutation+ (odds ratio, 3.66; P(trend)=0.049) and SCN5A mutation− (odds ratio, 3.75; P(trend)=8.54×10(−9)) subgroups. Furthermore, BrS patients without SCN5A mutations had more risk alleles than BrS patients with SCN5A mutations regardless of the range of polygenic risk scores. Three SNPs (rs4687718, rs7784776, and rs2968863) showed significant associations with the composite outcome (sudden cardiac arrest plus syncope, hazard ratio, 2.13, 1.48, and 0.41; P=0.02, 0.006, and 0.008, respectively). CONCLUSIONS: Our findings suggested that some SNPs associated with BrS or ECG traits exist across multiple populations. The cumulative risk of the BrS-related SNPs is similar to that in white BrS patients, but it appears to correlate with the absence of SCN5A mutations. |
| format | Online Article Text |
| id | pubmed-7439932 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2020 |
| publisher | Lippincott Williams & Wilkins |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-74399322020-09-04 Validation and Disease Risk Assessment of Previously Reported Genome-Wide Genetic Variants Associated With Brugada Syndrome: SADS-TW BrS Registry Jimmy Juang, Jyh-Ming Liu, Yen-Bin Julius Chen, Ching-Yu Yu, Qi-You Chattopadhyay, Amrita Lin, Lian-Yu Chen, Wen-Jone Yu, Chih-Chien Huang, Hui-Chun Ho, Li-Ting Lai, Ling-Ping Hwang, Juey-Jen Lin, Ting-Tse Liao, Min-Tsun Chen, Jien-Jiun Sherri Yeh, Shih-Fan Chuang, Jing-Yuan Yang, Dun-Hui Lin, Jiunn-Lee Lu, Tzu-Pin Chuang, Eric Y. Ackerman, Michael J. Circ Genom Precis Med Original Articles BACKGROUND: Brugada syndrome (BrS) is an oligogenic arrhythmic disease with increased risk of sudden cardiac arrest. Several BrS or ECG traits-related single-nucleotide polymorphisms (SNPs) were identified through previous genome-wide association studies in white patients. We aimed to validate these SNPs in BrS patients in the Taiwanese population, assessing the cumulative effect of risk alleles and the BrS-polygenic risk score in predicting cardiac events. METHODS: We genotyped 190 unrelated BrS patients using the TWB Array, and Taiwan Biobank was used as controls. SNPs not included in the array were imputed by IMPUTE2. Cox proportional hazards model was used to evaluate the associations between each particular SNP, the collective BrS-polygenic risk score, and clinical outcomes. RESULTS: Of the 88 previously reported SNPs, 22 were validated in Taiwanese BrS patients (P<0.05). Of the 22 SNPs, 2 (rs10428132 and rs9388451) were linked with susceptibility to BrS, 10 were SNPs previously reaching genome-wide significance, and 10 were SNPs associated with ECG traits. For the 3 most commonly reported SNPs, disease risk increased consistently with the number of risk alleles (odds ratio, 3.54; P(trend)=1.38×10(−9) for 5 risk alleles versus 1). Similar patterns were observed in both SCN5A mutation+ (odds ratio, 3.66; P(trend)=0.049) and SCN5A mutation− (odds ratio, 3.75; P(trend)=8.54×10(−9)) subgroups. Furthermore, BrS patients without SCN5A mutations had more risk alleles than BrS patients with SCN5A mutations regardless of the range of polygenic risk scores. Three SNPs (rs4687718, rs7784776, and rs2968863) showed significant associations with the composite outcome (sudden cardiac arrest plus syncope, hazard ratio, 2.13, 1.48, and 0.41; P=0.02, 0.006, and 0.008, respectively). CONCLUSIONS: Our findings suggested that some SNPs associated with BrS or ECG traits exist across multiple populations. The cumulative risk of the BrS-related SNPs is similar to that in white BrS patients, but it appears to correlate with the absence of SCN5A mutations. Lippincott Williams & Wilkins 2020-06-03 /pmc/articles/PMC7439932/ /pubmed/32490690 http://dx.doi.org/10.1161/CIRCGEN.119.002797 Text en © 2020 The Authors. Circulation: Genomic and Precision Medicine is published on behalf of the American Heart Association, Inc., by Wolters Kluwer Health, Inc. This is an open access article under the terms of the Creative Commons Attribution Non-Commercial-NoDerivs (https://creativecommons.org/licenses/by-nc-nd/4.0/) License, which permits use, distribution, and reproduction in any medium, provided that the original work is properly cited, the use is noncommercial, and no modifications or adaptations are made. |
| spellingShingle | Original Articles Jimmy Juang, Jyh-Ming Liu, Yen-Bin Julius Chen, Ching-Yu Yu, Qi-You Chattopadhyay, Amrita Lin, Lian-Yu Chen, Wen-Jone Yu, Chih-Chien Huang, Hui-Chun Ho, Li-Ting Lai, Ling-Ping Hwang, Juey-Jen Lin, Ting-Tse Liao, Min-Tsun Chen, Jien-Jiun Sherri Yeh, Shih-Fan Chuang, Jing-Yuan Yang, Dun-Hui Lin, Jiunn-Lee Lu, Tzu-Pin Chuang, Eric Y. Ackerman, Michael J. Validation and Disease Risk Assessment of Previously Reported Genome-Wide Genetic Variants Associated With Brugada Syndrome: SADS-TW BrS Registry |
| title | Validation and Disease Risk Assessment of Previously Reported Genome-Wide Genetic Variants Associated With Brugada Syndrome: SADS-TW BrS Registry |
| title_full | Validation and Disease Risk Assessment of Previously Reported Genome-Wide Genetic Variants Associated With Brugada Syndrome: SADS-TW BrS Registry |
| title_fullStr | Validation and Disease Risk Assessment of Previously Reported Genome-Wide Genetic Variants Associated With Brugada Syndrome: SADS-TW BrS Registry |
| title_full_unstemmed | Validation and Disease Risk Assessment of Previously Reported Genome-Wide Genetic Variants Associated With Brugada Syndrome: SADS-TW BrS Registry |
| title_short | Validation and Disease Risk Assessment of Previously Reported Genome-Wide Genetic Variants Associated With Brugada Syndrome: SADS-TW BrS Registry |
| title_sort | validation and disease risk assessment of previously reported genome-wide genetic variants associated with brugada syndrome: sads-tw brs registry |
| topic | Original Articles |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7439932/ https://www.ncbi.nlm.nih.gov/pubmed/32490690 http://dx.doi.org/10.1161/CIRCGEN.119.002797 |
| work_keys_str_mv | AT jimmyjuangjyhming validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT liuyenbin validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT juliuschenchingyu validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT yuqiyou validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT chattopadhyayamrita validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT linlianyu validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT chenwenjone validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT yuchihchien validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT huanghuichun validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT holiting validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT lailingping validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT hwangjueyjen validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT lintingtse validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT liaomintsun validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT chenjienjiun validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT sherriyehshihfan validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT chuangjingyuan validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT yangdunhui validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT linjiunnlee validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT lutzupin validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT chuangericy validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry AT ackermanmichaelj validationanddiseaseriskassessmentofpreviouslyreportedgenomewidegeneticvariantsassociatedwithbrugadasyndromesadstwbrsregistry |