Blood pressure (BP) is a major cardiovascular disease risk factor. To date, few variants associated with inter-individual BP variation have been identified. A genome-wide association study of systolic (SBP), diastolic BP (DBP), and hypertension in the CHARGE Consortium (n=29,136) identified 13 SNPs for SBP, 20 for DBP, and 10 for hypertension at p <4×10 -7 . The top 10 loci for SBP and DBP were incorporated into a risk score; mean BP and prevalence of hypertension increased in relation to number of risk alleles carried. When 10 CHARGE SNPs for each trait were meta-analyzed jointly with the Global BPgen Consortium (n=34,433), four CHARGE loci attained genome-wide significance (p<5×10 -8 ) for SBP (ATP2B1, CYP17A1, PLEKHA7, SH2B3), six for DBP (ATP2B1, CACNB2, CSK/ULK3, SH2B3, TBX3/TBX5, ULK4), and one for hypertension (ATP2B1). Identifying novel BP genes advances our understanding of BP regulation and highlights potential drug targets for the prevention or treatment of hypertension.High blood pressure affects about one third of adults and contributes to 13.5 million deaths worldwide each year and about half the global risk for stroke and ischemic heart disease. 1,2 Clinical trials, dating back more than forty years, have proven that drug treatment to lower blood pressure dramatically reduces the risk of cardiovascular events in people with hypertension. 3,4 The substantial (30-60 percent) 5 heritability of blood pressure has prompted extensive efforts to identify its genetic underpinnings. The search for genes associated with interindividual variation in blood pressure in the general population has used a variety of complementary approaches, which have yielded relatively few clues. Linkage and candidate gene studies, despite considerable knowledge about pathways that are critical to blood pressure homeostasis, have provided limited consistent evidence of blood pressure quantitative trait loci. 6,7,8 The study of families with rare Mendelian high or low blood pressure syndromes has identified mutations with gain or loss of function in about a dozen renal sodium regulatory genes. 9 Common variants in two renal sodium regulatory genes have been found to be associated with blood pressure in the general population. 10 The vast majority of the genetic contribution to variation in blood pressure, however, remains unexplained.Large-scale genome-wide association studies (GWAS), in which hundreds of thousands of common genetic variants are genotyped and analyzed for disease association, have shown great success in identifying genes associated with common diseases and traits. 11,12 The fact that six GWAS published to date, however, have not identified loci associated with blood pressure or hypertension at p<5×10 -8 , has raised concerns about the utility of this approach for these traits. 13,14,15,16,17,18 If blood pressure variation in the general population is due to multiple variants with small effects, very large study samples are needed to identify them. We established the Cohorts for Heart and Aging Research i...
