Genetic loci associated with prevalent and incident myocardial infarction and coronary heart disease in the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium

Julie Hahn; Yi Ping Fu; Michael R. Brown; Joshua C. Bis; Paul S. de Vries; Mary F. Feitosa; Lisa R. Yanek; Stefan Weiss; Franco Giulianini; Albert Vernon Smith; Xiuqing Guo; Traci M. Bartz; Diane M. Becker; Lewis C. Becker; Eric Boerwinkle; Jennifer A. Brody; Yii Der Ida Chen; Oscar H. Franco; Megan Grove; Tamara B. Harris; Albert Hofman; Shih Jen Hwang; Brian G. Kral; Lenore J. Launer; Marcello R.P. Markus; Kenneth M. Rice; Stephen S. Rich; Paul M. Ridker; Fernando Rivadeneira; Jerome I. Rotter; Nona Sotoodehnia; Kent D. Taylor; André G. Uitterlinden; Uwe Völker; Henry Völzke; Jie Yao; Daniel I. Chasman; Marcus Dörr; Vilmundur Gudnason; Rasika A. Mathias; Wendy Post; Bruce M. Psaty; Abbas Dehghan; Christopher J. O’Donnell; Alanna C. Morrison

doi:10.1371/journal.pone.0230035

Genetic loci associated with prevalent and incident myocardial infarction and coronary heart disease in the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium

Julie Hahn, Yi Ping Fu, Michael R. Brown, Joshua C. Bis, Paul S. de Vries, Mary F. Feitosa, Lisa R. Yanek, Stefan Weiss, Franco Giulianini, Albert Vernon Smith, Xiuqing Guo, Traci M. Bartz, Diane M. Becker, Lewis C. Becker, Eric Boerwinkle, Jennifer A. Brody, Yii Der Ida Chen, Oscar H. Franco, Megan Grove, Tamara B. HarrisAlbert Hofman, Shih Jen Hwang, Brian G. Kral, Lenore J. Launer, Marcello R.P. Markus, Kenneth M. Rice, Stephen S. Rich, Paul M. Ridker, Fernando Rivadeneira, Jerome I. Rotter, Nona Sotoodehnia, Kent D. Taylor, André G. Uitterlinden, Uwe Völker, Henry Völzke, Jie Yao, Daniel I. Chasman, Marcus Dörr, Vilmundur Gudnason, Rasika A. Mathias, Wendy Post, Bruce M. Psaty, Abbas Dehghan, Christopher J. O’Donnell, Alanna C. Morrison

School of Medicine

Research output: Contribution to journal › Article › peer-review

Abstract

Background Genome-wide association studies have identified multiple genomic loci associated with coronary artery disease, but most are common variants in non-coding regions that provide limited information on causal genes and etiology of the disease. To overcome the limited scope that common variants provide, we focused our investigation on low-frequency and rare sequence variations primarily residing in coding regions of the genome. Methods and results Using samples of individuals of European ancestry from ten cohorts within the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) consortium, both cross-sectional and prospective analyses were conducted to examine associations between genetic variants and myocardial infarction (MI), coronary heart disease (CHD), and all-cause mortality following these events. For prevalent events, a total of 27,349 participants of European ancestry, including 1831 prevalent MI cases and 2518 prevalent CHD cases were used. For incident cases, a total of 55,736 participants of European ancestry were included (3,031 incident MI cases and 5,425 incident CHD cases). There were 1,860 all-cause deaths among the 3,751 MI and CHD cases from six cohorts that contributed to the analysis of all-cause mortality. Single variant and gene-based analyses were performed separately in each cohort and then meta-analyzed for each outcome. A low-frequency intronic variant (rs988583) in PLCL1 was significantly associated with prevalent MI (OR = 1.80, 95% confidence interval: 1.43, 2.27; P = 7.12 × 10⁻⁷). We conducted gene-based burden tests for genes with a cumulative minor allele count (cMAC) > 5 and variants with minor allele frequency (MAF) < 5%. TMPRSS5 and LDLRAD1 were significantly associated with prevalent MI and CHD, respectively, and RC3H2 and ANGPTL4 were significantly associated with incident MI and CHD, respectively. No loci were significantly associated with all-cause mortality following a MI or CHD event. Conclusion This study identified one known locus (ANGPTL4) and four new loci (PLCL1, RC3H2, TMPRSS5, and LDLRAD1) associated with cardiovascular disease risk that warrant further investigation.

Original language	English (US)
Article number	e0230035
Journal	PloS one
Volume	15
Issue number	11 November
DOIs	https://doi.org/10.1371/journal.pone.0230035
State	Published - Nov 2020

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Hahn, J., Fu, Y. P., Brown, M. R., Bis, J. C., de Vries, P. S., Feitosa, M. F., Yanek, L. R., Weiss, S., Giulianini, F., Smith, A. V., Guo, X., Bartz, T. M., Becker, D. M., Becker, L. C., Boerwinkle, E., Brody, J. A., Chen, Y. D. I., Franco, O. H., Grove, M., ... Morrison, A. C. (2020). Genetic loci associated with prevalent and incident myocardial infarction and coronary heart disease in the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium. PloS one, 15(11 November), [e0230035]. https://doi.org/10.1371/journal.pone.0230035

Hahn, J, Fu, YP, Brown, MR, Bis, JC, de Vries, PS, Feitosa, MF, Yanek, LR, Weiss, S, Giulianini, F, Smith, AV, Guo, X, Bartz, TM, Becker, DM, Becker, LC, Boerwinkle, E, Brody, JA, Chen, YDI, Franco, OH, Grove, M, Harris, TB, Hofman, A, Hwang, SJ, Kral, BG, Launer, LJ, Markus, MRP, Rice, KM, Rich, SS, Ridker, PM, Rivadeneira, F, Rotter, JI, Sotoodehnia, N, Taylor, KD, Uitterlinden, AG, Völker, U, Völzke, H, Yao, J, Chasman, DI, Dörr, M, Gudnason, V, Mathias, RA , Post, W, Psaty, BM, Dehghan, A, O’Donnell, CJ & Morrison, AC 2020, 'Genetic loci associated with prevalent and incident myocardial infarction and coronary heart disease in the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium', PloS one, vol. 15, no. 11 November, e0230035. https://doi.org/10.1371/journal.pone.0230035

@article{a132f23ea5c3486ab64ee5b9cc48d655,

title = "Genetic loci associated with prevalent and incident myocardial infarction and coronary heart disease in the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium",

abstract = "Background Genome-wide association studies have identified multiple genomic loci associated with coronary artery disease, but most are common variants in non-coding regions that provide limited information on causal genes and etiology of the disease. To overcome the limited scope that common variants provide, we focused our investigation on low-frequency and rare sequence variations primarily residing in coding regions of the genome. Methods and results Using samples of individuals of European ancestry from ten cohorts within the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) consortium, both cross-sectional and prospective analyses were conducted to examine associations between genetic variants and myocardial infarction (MI), coronary heart disease (CHD), and all-cause mortality following these events. For prevalent events, a total of 27,349 participants of European ancestry, including 1831 prevalent MI cases and 2518 prevalent CHD cases were used. For incident cases, a total of 55,736 participants of European ancestry were included (3,031 incident MI cases and 5,425 incident CHD cases). There were 1,860 all-cause deaths among the 3,751 MI and CHD cases from six cohorts that contributed to the analysis of all-cause mortality. Single variant and gene-based analyses were performed separately in each cohort and then meta-analyzed for each outcome. A low-frequency intronic variant (rs988583) in PLCL1 was significantly associated with prevalent MI (OR = 1.80, 95% confidence interval: 1.43, 2.27; P = 7.12 × 10−7). We conducted gene-based burden tests for genes with a cumulative minor allele count (cMAC) > 5 and variants with minor allele frequency (MAF) < 5%. TMPRSS5 and LDLRAD1 were significantly associated with prevalent MI and CHD, respectively, and RC3H2 and ANGPTL4 were significantly associated with incident MI and CHD, respectively. No loci were significantly associated with all-cause mortality following a MI or CHD event. Conclusion This study identified one known locus (ANGPTL4) and four new loci (PLCL1, RC3H2, TMPRSS5, and LDLRAD1) associated with cardiovascular disease risk that warrant further investigation.",

author = "Julie Hahn and Fu, {Yi Ping} and Brown, {Michael R.} and Bis, {Joshua C.} and {de Vries}, {Paul S.} and Feitosa, {Mary F.} and Yanek, {Lisa R.} and Stefan Weiss and Franco Giulianini and Smith, {Albert Vernon} and Xiuqing Guo and Bartz, {Traci M.} and Becker, {Diane M.} and Becker, {Lewis C.} and Eric Boerwinkle and Brody, {Jennifer A.} and Chen, {Yii Der Ida} and Franco, {Oscar H.} and Megan Grove and Harris, {Tamara B.} and Albert Hofman and Hwang, {Shih Jen} and Kral, {Brian G.} and Launer, {Lenore J.} and Markus, {Marcello R.P.} and Rice, {Kenneth M.} and Rich, {Stephen S.} and Ridker, {Paul M.} and Fernando Rivadeneira and Rotter, {Jerome I.} and Nona Sotoodehnia and Taylor, {Kent D.} and Uitterlinden, {Andr{\'e} G.} and Uwe V{\"o}lker and Henry V{\"o}lzke and Jie Yao and Chasman, {Daniel I.} and Marcus D{\"o}rr and Vilmundur Gudnason and Mathias, {Rasika A.} and Wendy Post and Psaty, {Bruce M.} and Abbas Dehghan and O{\textquoteright}Donnell, {Christopher J.} and Morrison, {Alanna C.}",

note = "Funding Information: NorthwestGenomicsCenterattheUniversityof Washington,DepartmentofGenomeSciences, underU.S.FederalGovernmentcontractnumber HHSN268201100037CfromtheNationalHeart, Lung,andBloodInstitute.MESAandtheMESA SHAReprojectsareconductedandsupportedby theNationalHeart,Lung,andBloodInstitute (NHLBI)incollaborationwithMESAinvestigators. SupportforMESAisprovidedbycontracts 75N92020D00001,HHSN268201500003I,N01-HC-95159,75N92020D00005,N01-HC-95160, 75N92020D00002,N01-HC-95161, 75N92020D00003,N01-HC-95162, 75N92020D00006,N01-HC-95163, 75N92020D00004,N01-HC-95164, 75N92020D00007,N01-HC-95165,N01-HC- 95166,N01-HC-95167,N01-HC-95168,N01-HC- 95169,UL1-TR-000040,UL1-TR-001079,UL1- TR-001420.AlsosupportedinpartbytheNational CenterforAdvancingTranslationalSciences,CTSI grantUL1TR001881,andtheNationalInstituteof DiabetesandDigestiveandKidneyDisease DiabetesResearchCenter(DRC)grantDK063491 totheSouthernCaliforniaDiabetesEndocrinology ResearchCenter.FortheRotterdamStudy,the workwassupportedbytheErasmusMedical CenterandErasmusUniversity,Rotterdam;The NetherlandsOrganisationfortheHealthResearch andDevelopment(ZonMw);theResearchInstitute forDiseasesintheElderly(014-93-015,RIDE2); theMinistryofEducation,CultureandScience;the MinistryforHealth,WelfareandSports;the EuropeanCommission(DGXII);theMunicipalityof Rotterdam;TheNetherlandsOrganisationof ScientificResearch(NWO)(175.010.2005.011, 911-03-012);theNetherlandsGenomicsInitiative (NGI)(NWO050-060-810),theNetherlands OrganisationforScientificResearch(NWO)(veni 916.12.154).SHIPissupportedbytheGerman FederalMinistryofEducationandResearch (Bundesministeriumfu ¨r Bildungund Forschung (BMBF);grants01ZZ9603,01ZZ0103,and 01ZZ0403)andtheGermanResearchFoundation (DeutscheForschungsgemeinschaft(DFG);grant GR1912/5-1).TheStudyofHealthinPomerania (SHIP)andSHIP-TRENDarepartofthe CommunityMedicineResearchnet(CMR)ofthe Ernst-Moritz-ArndtUniversityGreifswald(EMAU) whichisfundedbytheBMBFaswellasthe MinistryforEducation,ScienceandCultureandthe MinistryofLabor,EqualOpportunities,andSocial AffairsoftheFederalStateofMecklenburg-West Pomerania.TheCMRencompassesseveral researchprojectsthatsharedatafromSHIP.The EMAUisamemberoftheCenterofKnowledge Interchange(CKI)programoftheSiemensAG. SNPtypingofSHIPandSHIP-TRENDusingthe Publisher Copyright: Copyright: This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 public domain dedication.",

year = "2020",

month = nov,

doi = "10.1371/journal.pone.0230035",

language = "English (US)",

volume = "15",

journal = "PLoS One",

issn = "1932-6203",

publisher = "Public Library of Science",

number = "11 November",

}

TY - JOUR

T1 - Genetic loci associated with prevalent and incident myocardial infarction and coronary heart disease in the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium

AU - Hahn, Julie

AU - Fu, Yi Ping

AU - Brown, Michael R.

AU - Bis, Joshua C.

AU - de Vries, Paul S.

AU - Feitosa, Mary F.

AU - Yanek, Lisa R.

AU - Weiss, Stefan

AU - Giulianini, Franco

AU - Smith, Albert Vernon

AU - Guo, Xiuqing

AU - Bartz, Traci M.

AU - Becker, Diane M.

AU - Becker, Lewis C.

AU - Boerwinkle, Eric

AU - Brody, Jennifer A.

AU - Chen, Yii Der Ida

AU - Franco, Oscar H.

AU - Grove, Megan

AU - Harris, Tamara B.

AU - Hofman, Albert

AU - Hwang, Shih Jen

AU - Kral, Brian G.

AU - Launer, Lenore J.

AU - Markus, Marcello R.P.

AU - Rice, Kenneth M.

AU - Rich, Stephen S.

AU - Ridker, Paul M.

AU - Rivadeneira, Fernando

AU - Rotter, Jerome I.

AU - Sotoodehnia, Nona

AU - Taylor, Kent D.

AU - Uitterlinden, André G.

AU - Völker, Uwe

AU - Völzke, Henry

AU - Yao, Jie

AU - Chasman, Daniel I.

AU - Dörr, Marcus

AU - Gudnason, Vilmundur

AU - Mathias, Rasika A.

AU - Post, Wendy

AU - Psaty, Bruce M.

AU - Dehghan, Abbas

AU - O’Donnell, Christopher J.

AU - Morrison, Alanna C.

N1 - Funding Information: NorthwestGenomicsCenterattheUniversityof Washington,DepartmentofGenomeSciences, underU.S.FederalGovernmentcontractnumber HHSN268201100037CfromtheNationalHeart, Lung,andBloodInstitute.MESAandtheMESA SHAReprojectsareconductedandsupportedby theNationalHeart,Lung,andBloodInstitute (NHLBI)incollaborationwithMESAinvestigators. SupportforMESAisprovidedbycontracts 75N92020D00001,HHSN268201500003I,N01-HC-95159,75N92020D00005,N01-HC-95160, 75N92020D00002,N01-HC-95161, 75N92020D00003,N01-HC-95162, 75N92020D00006,N01-HC-95163, 75N92020D00004,N01-HC-95164, 75N92020D00007,N01-HC-95165,N01-HC- 95166,N01-HC-95167,N01-HC-95168,N01-HC- 95169,UL1-TR-000040,UL1-TR-001079,UL1- TR-001420.AlsosupportedinpartbytheNational CenterforAdvancingTranslationalSciences,CTSI grantUL1TR001881,andtheNationalInstituteof DiabetesandDigestiveandKidneyDisease DiabetesResearchCenter(DRC)grantDK063491 totheSouthernCaliforniaDiabetesEndocrinology ResearchCenter.FortheRotterdamStudy,the workwassupportedbytheErasmusMedical CenterandErasmusUniversity,Rotterdam;The NetherlandsOrganisationfortheHealthResearch andDevelopment(ZonMw);theResearchInstitute forDiseasesintheElderly(014-93-015,RIDE2); theMinistryofEducation,CultureandScience;the MinistryforHealth,WelfareandSports;the EuropeanCommission(DGXII);theMunicipalityof Rotterdam;TheNetherlandsOrganisationof ScientificResearch(NWO)(175.010.2005.011, 911-03-012);theNetherlandsGenomicsInitiative (NGI)(NWO050-060-810),theNetherlands OrganisationforScientificResearch(NWO)(veni 916.12.154).SHIPissupportedbytheGerman FederalMinistryofEducationandResearch (Bundesministeriumfu ¨r Bildungund Forschung (BMBF);grants01ZZ9603,01ZZ0103,and 01ZZ0403)andtheGermanResearchFoundation (DeutscheForschungsgemeinschaft(DFG);grant GR1912/5-1).TheStudyofHealthinPomerania (SHIP)andSHIP-TRENDarepartofthe CommunityMedicineResearchnet(CMR)ofthe Ernst-Moritz-ArndtUniversityGreifswald(EMAU) whichisfundedbytheBMBFaswellasthe MinistryforEducation,ScienceandCultureandthe MinistryofLabor,EqualOpportunities,andSocial AffairsoftheFederalStateofMecklenburg-West Pomerania.TheCMRencompassesseveral researchprojectsthatsharedatafromSHIP.The EMAUisamemberoftheCenterofKnowledge Interchange(CKI)programoftheSiemensAG. SNPtypingofSHIPandSHIP-TRENDusingthe Publisher Copyright: Copyright: This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 public domain dedication.

PY - 2020/11

Y1 - 2020/11

N2 - Background Genome-wide association studies have identified multiple genomic loci associated with coronary artery disease, but most are common variants in non-coding regions that provide limited information on causal genes and etiology of the disease. To overcome the limited scope that common variants provide, we focused our investigation on low-frequency and rare sequence variations primarily residing in coding regions of the genome. Methods and results Using samples of individuals of European ancestry from ten cohorts within the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) consortium, both cross-sectional and prospective analyses were conducted to examine associations between genetic variants and myocardial infarction (MI), coronary heart disease (CHD), and all-cause mortality following these events. For prevalent events, a total of 27,349 participants of European ancestry, including 1831 prevalent MI cases and 2518 prevalent CHD cases were used. For incident cases, a total of 55,736 participants of European ancestry were included (3,031 incident MI cases and 5,425 incident CHD cases). There were 1,860 all-cause deaths among the 3,751 MI and CHD cases from six cohorts that contributed to the analysis of all-cause mortality. Single variant and gene-based analyses were performed separately in each cohort and then meta-analyzed for each outcome. A low-frequency intronic variant (rs988583) in PLCL1 was significantly associated with prevalent MI (OR = 1.80, 95% confidence interval: 1.43, 2.27; P = 7.12 × 10−7). We conducted gene-based burden tests for genes with a cumulative minor allele count (cMAC) > 5 and variants with minor allele frequency (MAF) < 5%. TMPRSS5 and LDLRAD1 were significantly associated with prevalent MI and CHD, respectively, and RC3H2 and ANGPTL4 were significantly associated with incident MI and CHD, respectively. No loci were significantly associated with all-cause mortality following a MI or CHD event. Conclusion This study identified one known locus (ANGPTL4) and four new loci (PLCL1, RC3H2, TMPRSS5, and LDLRAD1) associated with cardiovascular disease risk that warrant further investigation.

AB - Background Genome-wide association studies have identified multiple genomic loci associated with coronary artery disease, but most are common variants in non-coding regions that provide limited information on causal genes and etiology of the disease. To overcome the limited scope that common variants provide, we focused our investigation on low-frequency and rare sequence variations primarily residing in coding regions of the genome. Methods and results Using samples of individuals of European ancestry from ten cohorts within the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) consortium, both cross-sectional and prospective analyses were conducted to examine associations between genetic variants and myocardial infarction (MI), coronary heart disease (CHD), and all-cause mortality following these events. For prevalent events, a total of 27,349 participants of European ancestry, including 1831 prevalent MI cases and 2518 prevalent CHD cases were used. For incident cases, a total of 55,736 participants of European ancestry were included (3,031 incident MI cases and 5,425 incident CHD cases). There were 1,860 all-cause deaths among the 3,751 MI and CHD cases from six cohorts that contributed to the analysis of all-cause mortality. Single variant and gene-based analyses were performed separately in each cohort and then meta-analyzed for each outcome. A low-frequency intronic variant (rs988583) in PLCL1 was significantly associated with prevalent MI (OR = 1.80, 95% confidence interval: 1.43, 2.27; P = 7.12 × 10−7). We conducted gene-based burden tests for genes with a cumulative minor allele count (cMAC) > 5 and variants with minor allele frequency (MAF) < 5%. TMPRSS5 and LDLRAD1 were significantly associated with prevalent MI and CHD, respectively, and RC3H2 and ANGPTL4 were significantly associated with incident MI and CHD, respectively. No loci were significantly associated with all-cause mortality following a MI or CHD event. Conclusion This study identified one known locus (ANGPTL4) and four new loci (PLCL1, RC3H2, TMPRSS5, and LDLRAD1) associated with cardiovascular disease risk that warrant further investigation.

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UR - http://www.scopus.com/inward/citedby.url?scp=85096065183&partnerID=8YFLogxK

U2 - 10.1371/journal.pone.0230035

DO - 10.1371/journal.pone.0230035

M3 - Article

C2 - 33186364

AN - SCOPUS:85096065183

SN - 1932-6203

VL - 15

JO - PLoS One

JF - PLoS One

IS - 11 November

M1 - e0230035

ER -

Genetic loci associated with prevalent and incident myocardial infarction and coronary heart disease in the Cohorts for Heart and Aging Research in Genomic Epidemiology (CHARGE) Consortium

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