Common variants in HSPB7 and FRMD4B associated with advanced heart failure

Thomas P. Cappola; Mingyao Li; Jing He; Bonnie Ky; Joan Gilmore; Liming Qu; Brendan Keating; Muredach Reilly; Cecelia E. Kim; Joseph Glessner; Edward Frackelton; Hakon Hakonarson; Faisel Syed; Ana Hindes; Scot J. Matkovich; Sharon Cresci; Gerald W. Dorn

doi:10.1161/CIRCGENETICS.109.898395

Common variants in HSPB7 and FRMD4B associated with advanced heart failure

Thomas P. Cappola, Mingyao Li, Jing He, Bonnie Ky, Joan Gilmore, Liming Qu, Brendan Keating, Muredach Reilly, Cecelia E. Kim, Joseph Glessner, Edward Frackelton, Hakon Hakonarson, Faisel Syed, Ana Hindes, Scot J. Matkovich, Sharon Cresci, Gerald W. Dorn

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Abstract

Background-Heart failure results from abnormalities in multiple biological processes that contribute to cardiac dysfunction. We tested the hypothesis that inherited variation in genes of known importance to cardiovascular biology would thus contribute to heart failure risk. Methods and Results-We used the ITMAT/Broad/CARe cardiovascular single-nucleotide polymorphism array to screen referral populations of patients with advanced heart failure for variants in ≈2000 genes of predicted importance to cardiovascular biology. Our design was a 2-stage case-control study. In stage 1, genotypes in Caucasian patients with heart failure (n=1590; ejection fraction, 32±16%) were compared with those in unaffected controls (n=577; ejection fraction, 67±8%) who were recruited from the same referral centers. Associations were tested for independent replication in stage 2 (308 cases and 2314 controls). Two intronic single-nucleotide polymorphisms showed replicated associations with all-cause heart failure as follows: rs1739843 in HSPB7 (combined P=3.09×10 ^-6) and rs6787362 in FRMD4B (P=6.09×10^-6). For both single-nucleotide polymorphisms, the minor allele was protective. In subgroup analyses, rs1739843 associated with both ischemic and nonischemic heart failure, whereas rs6787362 associated principally with ischemic heart failure. Linkage disequilibrium surrounding rs1739843 suggested that the causal variant resides in a region containing HSPB7 and a neighboring gene, CLCNKA, whereas the causal variant near rs6787362 is probably within FRMD4B. Allele frequencies for these single-nucleotide polymorphisms were substantially different in African Americans (635 cases and 714 controls) and showed no association with heart failure in this population. Conclusions-Our findings identify regions containing HSPB7 and FRMD4B as novel susceptibility loci for advanced heart failure. More broadly, in an era of genome-wide association studies, we demonstrate how knowledge of candidate genes can be leveraged as a complementary strategy to discern the genetics of complex disorders. (Circ Cardiovasc Genet. 2010;3:147-154.)

Original language	English
Pages (from-to)	147-154
Number of pages	8
Journal	Circulation: Cardiovascular Genetics
Volume	3
Issue number	2
DOIs	https://doi.org/10.1161/CIRCGENETICS.109.898395
State	Published - Apr 2010

Keywords

Cardiomyopathy
Genetics
Heart failure

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10.1161/CIRCGENETICS.109.898395

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Cappola, T. P., Li, M., He, J., Ky, B., Gilmore, J., Qu, L., Keating, B., Reilly, M., Kim, C. E., Glessner, J., Frackelton, E., Hakonarson, H., Syed, F., Hindes, A., Matkovich, S. J., Cresci, S., & Dorn, G. W. (2010). Common variants in HSPB7 and FRMD4B associated with advanced heart failure. Circulation: Cardiovascular Genetics, 3(2), 147-154. https://doi.org/10.1161/CIRCGENETICS.109.898395

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title = "Common variants in HSPB7 and FRMD4B associated with advanced heart failure",

abstract = "Background-Heart failure results from abnormalities in multiple biological processes that contribute to cardiac dysfunction. We tested the hypothesis that inherited variation in genes of known importance to cardiovascular biology would thus contribute to heart failure risk. Methods and Results-We used the ITMAT/Broad/CARe cardiovascular single-nucleotide polymorphism array to screen referral populations of patients with advanced heart failure for variants in ≈2000 genes of predicted importance to cardiovascular biology. Our design was a 2-stage case-control study. In stage 1, genotypes in Caucasian patients with heart failure (n=1590; ejection fraction, 32±16%) were compared with those in unaffected controls (n=577; ejection fraction, 67±8%) who were recruited from the same referral centers. Associations were tested for independent replication in stage 2 (308 cases and 2314 controls). Two intronic single-nucleotide polymorphisms showed replicated associations with all-cause heart failure as follows: rs1739843 in HSPB7 (combined P=3.09×10 -6) and rs6787362 in FRMD4B (P=6.09×10-6). For both single-nucleotide polymorphisms, the minor allele was protective. In subgroup analyses, rs1739843 associated with both ischemic and nonischemic heart failure, whereas rs6787362 associated principally with ischemic heart failure. Linkage disequilibrium surrounding rs1739843 suggested that the causal variant resides in a region containing HSPB7 and a neighboring gene, CLCNKA, whereas the causal variant near rs6787362 is probably within FRMD4B. Allele frequencies for these single-nucleotide polymorphisms were substantially different in African Americans (635 cases and 714 controls) and showed no association with heart failure in this population. Conclusions-Our findings identify regions containing HSPB7 and FRMD4B as novel susceptibility loci for advanced heart failure. More broadly, in an era of genome-wide association studies, we demonstrate how knowledge of candidate genes can be leveraged as a complementary strategy to discern the genetics of complex disorders. (Circ Cardiovasc Genet. 2010;3:147-154.)",

keywords = "Cardiomyopathy, Genetics, Heart failure",

author = "Cappola, {Thomas P.} and Mingyao Li and Jing He and Bonnie Ky and Joan Gilmore and Liming Qu and Brendan Keating and Muredach Reilly and Kim, {Cecelia E.} and Joseph Glessner and Edward Frackelton and Hakon Hakonarson and Faisel Syed and Ana Hindes and Matkovich, {Scot J.} and Sharon Cresci and Dorn, {Gerald W.}",

year = "2010",

month = apr,

doi = "10.1161/CIRCGENETICS.109.898395",

language = "English",

volume = "3",

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Cappola, TP, Li, M, He, J, Ky, B, Gilmore, J, Qu, L, Keating, B, Reilly, M, Kim, CE, Glessner, J, Frackelton, E, Hakonarson, H, Syed, F, Hindes, A, Matkovich, SJ, Cresci, S & Dorn, GW 2010, 'Common variants in HSPB7 and FRMD4B associated with advanced heart failure', Circulation: Cardiovascular Genetics, vol. 3, no. 2, pp. 147-154. https://doi.org/10.1161/CIRCGENETICS.109.898395

TY - JOUR

T1 - Common variants in HSPB7 and FRMD4B associated with advanced heart failure

AU - Cappola, Thomas P.

AU - Li, Mingyao

AU - He, Jing

AU - Ky, Bonnie

AU - Gilmore, Joan

AU - Qu, Liming

AU - Keating, Brendan

AU - Reilly, Muredach

AU - Kim, Cecelia E.

AU - Glessner, Joseph

AU - Frackelton, Edward

AU - Hakonarson, Hakon

AU - Syed, Faisel

AU - Hindes, Ana

AU - Matkovich, Scot J.

AU - Cresci, Sharon

AU - Dorn, Gerald W.

PY - 2010/4

Y1 - 2010/4

N2 - Background-Heart failure results from abnormalities in multiple biological processes that contribute to cardiac dysfunction. We tested the hypothesis that inherited variation in genes of known importance to cardiovascular biology would thus contribute to heart failure risk. Methods and Results-We used the ITMAT/Broad/CARe cardiovascular single-nucleotide polymorphism array to screen referral populations of patients with advanced heart failure for variants in ≈2000 genes of predicted importance to cardiovascular biology. Our design was a 2-stage case-control study. In stage 1, genotypes in Caucasian patients with heart failure (n=1590; ejection fraction, 32±16%) were compared with those in unaffected controls (n=577; ejection fraction, 67±8%) who were recruited from the same referral centers. Associations were tested for independent replication in stage 2 (308 cases and 2314 controls). Two intronic single-nucleotide polymorphisms showed replicated associations with all-cause heart failure as follows: rs1739843 in HSPB7 (combined P=3.09×10 -6) and rs6787362 in FRMD4B (P=6.09×10-6). For both single-nucleotide polymorphisms, the minor allele was protective. In subgroup analyses, rs1739843 associated with both ischemic and nonischemic heart failure, whereas rs6787362 associated principally with ischemic heart failure. Linkage disequilibrium surrounding rs1739843 suggested that the causal variant resides in a region containing HSPB7 and a neighboring gene, CLCNKA, whereas the causal variant near rs6787362 is probably within FRMD4B. Allele frequencies for these single-nucleotide polymorphisms were substantially different in African Americans (635 cases and 714 controls) and showed no association with heart failure in this population. Conclusions-Our findings identify regions containing HSPB7 and FRMD4B as novel susceptibility loci for advanced heart failure. More broadly, in an era of genome-wide association studies, we demonstrate how knowledge of candidate genes can be leveraged as a complementary strategy to discern the genetics of complex disorders. (Circ Cardiovasc Genet. 2010;3:147-154.)

AB - Background-Heart failure results from abnormalities in multiple biological processes that contribute to cardiac dysfunction. We tested the hypothesis that inherited variation in genes of known importance to cardiovascular biology would thus contribute to heart failure risk. Methods and Results-We used the ITMAT/Broad/CARe cardiovascular single-nucleotide polymorphism array to screen referral populations of patients with advanced heart failure for variants in ≈2000 genes of predicted importance to cardiovascular biology. Our design was a 2-stage case-control study. In stage 1, genotypes in Caucasian patients with heart failure (n=1590; ejection fraction, 32±16%) were compared with those in unaffected controls (n=577; ejection fraction, 67±8%) who were recruited from the same referral centers. Associations were tested for independent replication in stage 2 (308 cases and 2314 controls). Two intronic single-nucleotide polymorphisms showed replicated associations with all-cause heart failure as follows: rs1739843 in HSPB7 (combined P=3.09×10 -6) and rs6787362 in FRMD4B (P=6.09×10-6). For both single-nucleotide polymorphisms, the minor allele was protective. In subgroup analyses, rs1739843 associated with both ischemic and nonischemic heart failure, whereas rs6787362 associated principally with ischemic heart failure. Linkage disequilibrium surrounding rs1739843 suggested that the causal variant resides in a region containing HSPB7 and a neighboring gene, CLCNKA, whereas the causal variant near rs6787362 is probably within FRMD4B. Allele frequencies for these single-nucleotide polymorphisms were substantially different in African Americans (635 cases and 714 controls) and showed no association with heart failure in this population. Conclusions-Our findings identify regions containing HSPB7 and FRMD4B as novel susceptibility loci for advanced heart failure. More broadly, in an era of genome-wide association studies, we demonstrate how knowledge of candidate genes can be leveraged as a complementary strategy to discern the genetics of complex disorders. (Circ Cardiovasc Genet. 2010;3:147-154.)

KW - Cardiomyopathy

KW - Genetics

KW - Heart failure

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U2 - 10.1161/CIRCGENETICS.109.898395

DO - 10.1161/CIRCGENETICS.109.898395

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SN - 1942-325X

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EP - 154

JO - Circulation: Cardiovascular Genetics

JF - Circulation: Cardiovascular Genetics

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ER -

Common variants in HSPB7 and FRMD4B associated with advanced heart failure

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