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Hypertrophy-Associated Polymorphisms Ascertained in a Founder Cohort Applied to Heart Failure Risk and Mortality

A three‐stage approach was undertaken using genome‐wide, case‐control, and case‐only association studies to identify genetic variants associated with heart failure mortality. In an Amish founder population (n = 851), cardiac hypertrophy, a trait integral to the adaptive response to failure, was foun...

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Published in:	Clinical and translational science 2011-02, Vol.4 (1), p.17-23
Main Authors:	Parsa, Afshin, Chang, Yen-Pei C., Kelly, Reagan J., Corretti, Mary C., Ryan, Kathleen A., Robinson, Shawn W., Gottlieb, Stephen S., Kardia, Sharon L.R., Shuldiner, Alan R., Liggett, Stephen B.
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Language:	English
Subjects:	Adult Aged Aged, 80 and over Base Sequence Cardiomegaly - complications Cardiomegaly - diagnostic imaging Cardiomegaly - genetics Cohort Studies Demography Ethnic Groups - genetics Female Founder Effect Genetic Predisposition to Disease genetics heart failure Heart Failure - complications Heart Failure - diagnostic imaging Heart Failure - genetics Heart Failure - mortality Heart Ventricles - pathology Humans hypertrophy Male Middle Aged mortality Organ Size Polymorphism, Single Nucleotide - drug effects Polymorphism, Single Nucleotide - genetics Risk Factors Sequence Homology, Nucleic Acid Short Interspersed Nucleotide Elements - genetics signal transduction Ultrasonography Young Adult
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creator	Parsa, Afshin Chang, Yen-Pei C. Kelly, Reagan J. Corretti, Mary C. Ryan, Kathleen A. Robinson, Shawn W. Gottlieb, Stephen S. Kardia, Sharon L.R. Shuldiner, Alan R. Liggett, Stephen B.
description	A three‐stage approach was undertaken using genome‐wide, case‐control, and case‐only association studies to identify genetic variants associated with heart failure mortality. In an Amish founder population (n = 851), cardiac hypertrophy, a trait integral to the adaptive response to failure, was found to be heritable (h2= 0.28, p = 0.0002) and GWAS revealed 21 candidate hypertrophy SNPs. In a case (n = 1,610)‐control (n = 463) study in unrelated Caucasians, one of the SNPs associated with hypertrophy (rs2207418, p = 8 × 10−6), was associated with heart failure, RR = 1.85(1.25–2.73, p = 0.0019). In heart failure cases rs2207418 was associated with increased mortality, HR = 1.51(1.20–1.97, p = 0.0004). There was consistency between studies, with the GG allele being associated with increased ventricular mass (˜13 g/m2) in the Amish, heart failure risk, and heart failure mortality. This SNP is in a gene desert of chromosome 20p12. Five genes are within 2.0 mbp of rs2207418 but with low LD between their SNPs and rs2207418. A region near this SNP is highly conserved in multiple vertebrates (lod score = 1,208). This conservation and the internal consistency across studies suggests that this region has biologic importance in heart failure, potentially acting as an enhancer or repressor element. rs2207418 may be useful for predicting a more progressive form of heart failure that may require aggressive therapy. Clin Trans Sci 2011; Volume 4: 17–23
doi_str_mv	10.1111/j.1752-8062.2010.00251.x
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This conservation and the internal consistency across studies suggests that this region has biologic importance in heart failure, potentially acting as an enhancer or repressor element. rs2207418 may be useful for predicting a more progressive form of heart failure that may require aggressive therapy. 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In an Amish founder population (n = 851), cardiac hypertrophy, a trait integral to the adaptive response to failure, was found to be heritable (h2= 0.28, p = 0.0002) and GWAS revealed 21 candidate hypertrophy SNPs. In a case (n = 1,610)‐control (n = 463) study in unrelated Caucasians, one of the SNPs associated with hypertrophy (rs2207418, p = 8 × 10−6), was associated with heart failure, RR = 1.85(1.25–2.73, p = 0.0019). In heart failure cases rs2207418 was associated with increased mortality, HR = 1.51(1.20–1.97, p = 0.0004). There was consistency between studies, with the GG allele being associated with increased ventricular mass (˜13 g/m2) in the Amish, heart failure risk, and heart failure mortality. This SNP is in a gene desert of chromosome 20p12. Five genes are within 2.0 mbp of rs2207418 but with low LD between their SNPs and rs2207418. A region near this SNP is highly conserved in multiple vertebrates (lod score = 1,208). This conservation and the internal consistency across studies suggests that this region has biologic importance in heart failure, potentially acting as an enhancer or repressor element. rs2207418 may be useful for predicting a more progressive form of heart failure that may require aggressive therapy. 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In an Amish founder population (n = 851), cardiac hypertrophy, a trait integral to the adaptive response to failure, was found to be heritable (h2= 0.28, p = 0.0002) and GWAS revealed 21 candidate hypertrophy SNPs. In a case (n = 1,610)‐control (n = 463) study in unrelated Caucasians, one of the SNPs associated with hypertrophy (rs2207418, p = 8 × 10−6), was associated with heart failure, RR = 1.85(1.25–2.73, p = 0.0019). In heart failure cases rs2207418 was associated with increased mortality, HR = 1.51(1.20–1.97, p = 0.0004). There was consistency between studies, with the GG allele being associated with increased ventricular mass (˜13 g/m2) in the Amish, heart failure risk, and heart failure mortality. This SNP is in a gene desert of chromosome 20p12. Five genes are within 2.0 mbp of rs2207418 but with low LD between their SNPs and rs2207418. A region near this SNP is highly conserved in multiple vertebrates (lod score = 1,208). This conservation and the internal consistency across studies suggests that this region has biologic importance in heart failure, potentially acting as an enhancer or repressor element. rs2207418 may be useful for predicting a more progressive form of heart failure that may require aggressive therapy. Clin Trans Sci 2011; Volume 4: 17–23</abstract><cop>Malden, USA</cop><pub>Blackwell Publishing Inc</pub><pmid>21348951</pmid><doi>10.1111/j.1752-8062.2010.00251.x</doi><tpages>7</tpages><oa>free_for_read</oa></addata></record>
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subjects	Adult Aged Aged, 80 and over Base Sequence Cardiomegaly - complications Cardiomegaly - diagnostic imaging Cardiomegaly - genetics Cohort Studies Demography Ethnic Groups - genetics Female Founder Effect Genetic Predisposition to Disease genetics heart failure Heart Failure - complications Heart Failure - diagnostic imaging Heart Failure - genetics Heart Failure - mortality Heart Ventricles - pathology Humans hypertrophy Male Middle Aged mortality Organ Size Polymorphism, Single Nucleotide - drug effects Polymorphism, Single Nucleotide - genetics Risk Factors Sequence Homology, Nucleic Acid Short Interspersed Nucleotide Elements - genetics signal transduction Ultrasonography Young Adult
title	Hypertrophy-Associated Polymorphisms Ascertained in a Founder Cohort Applied to Heart Failure Risk and Mortality
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