TY - JOUR
T1 - Genome-Wide Meta-Analyses of Plasma Renin Activity and Concentration Reveal Association with the Kininogen 1 and Prekallikrein Genes
AU - Lieb, Wolfgang
AU - Chen, Ming-Huei
AU - Teumer, Alexander
AU - de Boer, Rudolf A
AU - Lin, Honghuang
AU - Fox, Ervin R
AU - Musani, Solomon K
AU - Wilson, James G
AU - Wang, Thomas J
AU - Völzke, Henry
AU - Petersen, Ann-Kristin
AU - Meisinger, Christine
AU - Nauck, Matthias
AU - Schlesinger, Sabrina
AU - Li, Yong
AU - Ménard, Joël
AU - Hercberg, Serge
AU - Wichmann, H-Erich
AU - Völker, Uwe
AU - Rawal, Rajesh
AU - Bidlingmaier, Martin
AU - Hannemann, Anke
AU - Dörr, Marcus
AU - Rettig, Rainer
AU - van Gilst, Wiek H
AU - van Veldhuisen, Dirk J
AU - Bakker, Stephan J L
AU - Navis, Gerjan
AU - Wallaschofski, Henri
AU - Meneton, Pierre
AU - van der Harst, Pim
AU - Reincke, Martin
AU - Vasan, Ramachandran S
AU - CKDGen Consortium, ICBP, EchoGen Consortium
PY - 2015/2
Y1 - 2015/2
N2 - BACKGROUND: -The renin-angiotensin-aldosterone-system (RAAS) is critical for regulation of blood pressure and fluid balance and influences cardiovascular remodeling. Dysregulation of the RAAS contributes to cardiovascular and renal morbidity. The genetic architecture of circulating RAAS components is incompletely understood.METHODS AND RESULTS: -We meta-analyzed genome-wide association data for plasma renin activity (n=5,275), plasma renin concentrations (n=8,014) and circulating aldosterone (n=13,289) from up to four population-based cohorts of European and European-American ancestry, and assessed replication of the top results in an independent sample (n=6,487). Single nucleotide polymorphisms (SNPs) in two independent loci displayed associations with plasma renin activity at genome-wide significance (p<5x10(-8)). A third locus was close to this threshold (rs4253311 in kallikrein B [KLKB1], p=5.5x10(-8)). Two of these loci replicated in an independent sample for both plasma renin and aldosterone concentrations (SNP rs5030062 in kininogen 1 [KNG1]: p=0.001 for plasma renin, p=0.024 for plasma aldosterone concentration; rs4253311 with p<0.001 for both plasma renin and aldosterone concentration). SNPs in the NEBL gene reached genome-wide significance for plasma renin concentration in the discovery sample (top SNP rs3915911, p=8.81x10(-9)), but did not replicate (p=0.81). No locus reached genome-wide significance for aldosterone. SNPs rs5030062 and rs4253311 were not related to blood pressure or renal traits; in a companion study, variants in the kallikrein B locus were associated with B-type natriuretic peptide concentrations in African-Americans.CONCLUSIONS: -We identified two genetic loci (kininogen 1 and kallikrein B) influencing key components of the RAAS, consistent with the close interrelation between the kallikrein-kinin system and the RAAS.
AB - BACKGROUND: -The renin-angiotensin-aldosterone-system (RAAS) is critical for regulation of blood pressure and fluid balance and influences cardiovascular remodeling. Dysregulation of the RAAS contributes to cardiovascular and renal morbidity. The genetic architecture of circulating RAAS components is incompletely understood.METHODS AND RESULTS: -We meta-analyzed genome-wide association data for plasma renin activity (n=5,275), plasma renin concentrations (n=8,014) and circulating aldosterone (n=13,289) from up to four population-based cohorts of European and European-American ancestry, and assessed replication of the top results in an independent sample (n=6,487). Single nucleotide polymorphisms (SNPs) in two independent loci displayed associations with plasma renin activity at genome-wide significance (p<5x10(-8)). A third locus was close to this threshold (rs4253311 in kallikrein B [KLKB1], p=5.5x10(-8)). Two of these loci replicated in an independent sample for both plasma renin and aldosterone concentrations (SNP rs5030062 in kininogen 1 [KNG1]: p=0.001 for plasma renin, p=0.024 for plasma aldosterone concentration; rs4253311 with p<0.001 for both plasma renin and aldosterone concentration). SNPs in the NEBL gene reached genome-wide significance for plasma renin concentration in the discovery sample (top SNP rs3915911, p=8.81x10(-9)), but did not replicate (p=0.81). No locus reached genome-wide significance for aldosterone. SNPs rs5030062 and rs4253311 were not related to blood pressure or renal traits; in a companion study, variants in the kallikrein B locus were associated with B-type natriuretic peptide concentrations in African-Americans.CONCLUSIONS: -We identified two genetic loci (kininogen 1 and kallikrein B) influencing key components of the RAAS, consistent with the close interrelation between the kallikrein-kinin system and the RAAS.
KW - aldosterone
KW - genome-wide association study
KW - renin-angiotensin system
KW - ANGIOTENSIN-ALDOSTERONE SYSTEM
KW - METABOLIC SYNDROME
KW - CONVERTING ENZYME
KW - CARDIAC STRUCTURE
KW - BLOOD-PRESSURE
KW - GS-ALPHA
KW - HYPERTENSION
KW - POPULATION
KW - DISEASE
KW - HEART
U2 - 10.1161/CIRCGENETICS.114.000613
DO - 10.1161/CIRCGENETICS.114.000613
M3 - Article
C2 - 25477429
SN - 1942-325X
VL - 8
SP - 131
EP - 140
JO - Circulation-Cardiovascular Genetics
JF - Circulation-Cardiovascular Genetics
IS - 1
ER -