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In silico mapping of coronary artery disease genes. / Zorkoltseva, I. V.; Belonogova, N. M.; Svishcheva, G. R. и др.

в: Вавиловский журнал генетики и селекции, Том 23, № 8, 01.08.2019, стр. 1037-1046.

Результаты исследований: Научные публикации в периодических изданияхстатьяРецензирование

Harvard

Zorkoltseva, IV, Belonogova, NM, Svishcheva, GR, Kirichenko, AV & Axenovich, TI 2019, 'In silico mapping of coronary artery disease genes', Вавиловский журнал генетики и селекции, Том. 23, № 8, стр. 1037-1046. https://doi.org/10.18699/VJ19.585

APA

Zorkoltseva, I. V., Belonogova, N. M., Svishcheva, G. R., Kirichenko, A. V., & Axenovich, T. I. (2019). In silico mapping of coronary artery disease genes. Вавиловский журнал генетики и селекции, 23(8), 1037-1046. https://doi.org/10.18699/VJ19.585

Vancouver

Zorkoltseva IV, Belonogova NM, Svishcheva GR, Kirichenko AV, Axenovich TI. In silico mapping of coronary artery disease genes. Вавиловский журнал генетики и селекции. 2019 авг. 1;23(8):1037-1046. doi: 10.18699/VJ19.585

Author

Zorkoltseva, I. V. ; Belonogova, N. M. ; Svishcheva, G. R. и др. / In silico mapping of coronary artery disease genes. в: Вавиловский журнал генетики и селекции. 2019 ; Том 23, № 8. стр. 1037-1046.

BibTeX

@article{b93a0a0bb4cf4c85bfdb4369e59fbd26,
title = "In silico mapping of coronary artery disease genes",
abstract = "To date, more than 100 loci associated with coronary artery disease (CAD) have been detected in large-scale genomewide studies. For some of the several hundreds of genes located in these loci, roles in the pathogenesis of the disease have been shown. However, the genetic mechanisms and specific genes controlling this disease are still not fully understood. This study is aimed at in silico search for new CAD genes. We performed a gene-based association analysis, where all polymorphic variants within a gene are analyzed simultaneously. The analysis was based on the results of the genome-wide association studies (GWAS) available from the open databases MICAD (120,575 people, 85,112 markers) and UK Biobank (337,199 people, 10,894,597 markers). We used the sumFREGAT package implementing a wide range of new methods for gene-based association analysis using summary statistics. We found 88 genes demonstrating significant gene-based associations. Forty-four of the identified genes were already known as CAD genes. Furthermore, we identified 28 additional genes in the known CAD loci. They can be considered as new candidate genes. Finally, we identified sixteen new genes (AGPAT4, ARHGEF12, BDP1, DHX58, EHBP1, FBF1, HSPB9, NPBWR2, PDLIM5, PLCB3, PLEKHM2, POU2F3, PRKD2, TMEM136, TTC29 and UTP20) outside the known loci. Information about the functional role of these genes allows us to consider many of them as candidates for CAD. The 41 identified genes did not have significant GWAS signals and they were identified only due to simultaneous consideration of all variants within the gene in the framework of gene-based analysis. These results demonstrate that gene-based association analysis is a powerful tool for gene mapping. The method can utilize huge amounts of GWAS results accumulated in the world to map different traits and diseases. This type of studies is widely available, as it does not require additional material costs. Key words: coronary artery disease; gene-based association analysis; genome-wide association analysis; summary statistics; in silico mapping.",
keywords = "Coronary artery disease, Gene-based association analysis, Genome-wide association analysis, In silico mapping, Summary statistics, coronary artery disease, MIGRATION, PATHWAYS, gene-based association analysis, summary statistics, VARIANTS, RISK, PCSK9, LOCI, SCALE ASSOCIATION ANALYSIS, BLOOD-PRESSURE, HERITABILITY, in silica mapping, LD SCORE REGRESSION, genome-wide association analysis",
author = "Zorkoltseva, {I. V.} and Belonogova, {N. M.} and Svishcheva, {G. R.} and Kirichenko, {A. V.} and Axenovich, {T. I.}",
year = "2019",
month = aug,
day = "1",
doi = "10.18699/VJ19.585",
language = "English",
volume = "23",
pages = "1037--1046",
journal = "Вавиловский журнал генетики и селекции",
issn = "2500-0462",
publisher = "Institute of Cytology and Genetics of Siberian Branch of the Russian Academy of Sciences",
number = "8",

}

RIS

TY - JOUR

T1 - In silico mapping of coronary artery disease genes

AU - Zorkoltseva, I. V.

AU - Belonogova, N. M.

AU - Svishcheva, G. R.

AU - Kirichenko, A. V.

AU - Axenovich, T. I.

PY - 2019/8/1

Y1 - 2019/8/1

N2 - To date, more than 100 loci associated with coronary artery disease (CAD) have been detected in large-scale genomewide studies. For some of the several hundreds of genes located in these loci, roles in the pathogenesis of the disease have been shown. However, the genetic mechanisms and specific genes controlling this disease are still not fully understood. This study is aimed at in silico search for new CAD genes. We performed a gene-based association analysis, where all polymorphic variants within a gene are analyzed simultaneously. The analysis was based on the results of the genome-wide association studies (GWAS) available from the open databases MICAD (120,575 people, 85,112 markers) and UK Biobank (337,199 people, 10,894,597 markers). We used the sumFREGAT package implementing a wide range of new methods for gene-based association analysis using summary statistics. We found 88 genes demonstrating significant gene-based associations. Forty-four of the identified genes were already known as CAD genes. Furthermore, we identified 28 additional genes in the known CAD loci. They can be considered as new candidate genes. Finally, we identified sixteen new genes (AGPAT4, ARHGEF12, BDP1, DHX58, EHBP1, FBF1, HSPB9, NPBWR2, PDLIM5, PLCB3, PLEKHM2, POU2F3, PRKD2, TMEM136, TTC29 and UTP20) outside the known loci. Information about the functional role of these genes allows us to consider many of them as candidates for CAD. The 41 identified genes did not have significant GWAS signals and they were identified only due to simultaneous consideration of all variants within the gene in the framework of gene-based analysis. These results demonstrate that gene-based association analysis is a powerful tool for gene mapping. The method can utilize huge amounts of GWAS results accumulated in the world to map different traits and diseases. This type of studies is widely available, as it does not require additional material costs. Key words: coronary artery disease; gene-based association analysis; genome-wide association analysis; summary statistics; in silico mapping.

AB - To date, more than 100 loci associated with coronary artery disease (CAD) have been detected in large-scale genomewide studies. For some of the several hundreds of genes located in these loci, roles in the pathogenesis of the disease have been shown. However, the genetic mechanisms and specific genes controlling this disease are still not fully understood. This study is aimed at in silico search for new CAD genes. We performed a gene-based association analysis, where all polymorphic variants within a gene are analyzed simultaneously. The analysis was based on the results of the genome-wide association studies (GWAS) available from the open databases MICAD (120,575 people, 85,112 markers) and UK Biobank (337,199 people, 10,894,597 markers). We used the sumFREGAT package implementing a wide range of new methods for gene-based association analysis using summary statistics. We found 88 genes demonstrating significant gene-based associations. Forty-four of the identified genes were already known as CAD genes. Furthermore, we identified 28 additional genes in the known CAD loci. They can be considered as new candidate genes. Finally, we identified sixteen new genes (AGPAT4, ARHGEF12, BDP1, DHX58, EHBP1, FBF1, HSPB9, NPBWR2, PDLIM5, PLCB3, PLEKHM2, POU2F3, PRKD2, TMEM136, TTC29 and UTP20) outside the known loci. Information about the functional role of these genes allows us to consider many of them as candidates for CAD. The 41 identified genes did not have significant GWAS signals and they were identified only due to simultaneous consideration of all variants within the gene in the framework of gene-based analysis. These results demonstrate that gene-based association analysis is a powerful tool for gene mapping. The method can utilize huge amounts of GWAS results accumulated in the world to map different traits and diseases. This type of studies is widely available, as it does not require additional material costs. Key words: coronary artery disease; gene-based association analysis; genome-wide association analysis; summary statistics; in silico mapping.

KW - Coronary artery disease

KW - Gene-based association analysis

KW - Genome-wide association analysis

KW - In silico mapping

KW - Summary statistics

KW - coronary artery disease

KW - MIGRATION

KW - PATHWAYS

KW - gene-based association analysis

KW - summary statistics

KW - VARIANTS

KW - RISK

KW - PCSK9

KW - LOCI

KW - SCALE ASSOCIATION ANALYSIS

KW - BLOOD-PRESSURE

KW - HERITABILITY

KW - in silica mapping

KW - LD SCORE REGRESSION

KW - genome-wide association analysis

UR - http://www.scopus.com/inward/record.url?scp=85081958587&partnerID=8YFLogxK

U2 - 10.18699/VJ19.585

DO - 10.18699/VJ19.585

M3 - Article

AN - SCOPUS:85081958587

VL - 23

SP - 1037

EP - 1046

JO - Вавиловский журнал генетики и селекции

JF - Вавиловский журнал генетики и селекции

SN - 2500-0462

IS - 8

ER -

ID: 23878617