Abstract

A genetic epidemiology network of 9 centers, including Boston University/Framingham, will study genetic and interacting non-genetic determinants of hypertension. Previously collected data on hypertension and family history in white subjects from the Framingham Study and the Family Heart Study, and in black subjects at other sites, allow the identification of a large and equal sample of black and non-black families with 2+ hypertensive siblings, untreated relatives and controls (total 4,600 subjects) for genetic association and sibship linkage studies (to test 20 candidate genes and anonymous markers totalling about 750,000 genotype determinations); as well as a rich battery of epidemiologic analyses assessing family history and genotype information in combination with important non-genetic factors. The data coordinating center, four field centers (including Framingham), and biochemistry lab center of the Family Heart Study (""""""""FHS"""""""") plus two additional black field centers and DNA lab center form this network. The investigators in this network have published major findings regarding the genetics and epidemiology of hypertension and state-of-the-art technology in molecular biology, biochemistry, epidemiology, and specialized statistics for genetic epidemiology. These investigators have a proven track record of productive collaboration between institutions. The study design in this proposal takes full advantage of strong collaboration both within this network and between this and other networks operating under the same cooperative agreement. From a combined base population of over 20,000 screened probands, a sample of l,200 sibships have been indexed with two or more siblings having hypertension diagnosed before age 60. These sibships have been chosen to be equally divided into subgroups by race (black and non-black) and severity of hypertension (severe and mild) and can be further stratified by other pertinent factors (body mass index, plasma lipids, age of onset of hypertension, etc.). The choice of methods (genetic association and model-free sibship linkage) and large sample size with ability to analyze within more homogeneous subgroups provide good power to detect specific genetic loci promoting hypertension despite considerable heterogeneity. Replication studies in independent populations (these subjects versus previously studies Utah sibships and versus other collaborative Networks) will allow the confirmation of genetic loci for genes promoting hypertension. Loci found by other networks will also be rapidly tested in our subjects for confirmation. Epidemiological analyses of persons with and without one or more confirmed genes for hypertension in combination with non-genetic factors and intermediate phenotypes will identify gene- environment interactions and specific lifestyle factors whose presence or absence seem to help determine the likelihood of expressing specific genetic predispositions to hypertension.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Cooperative Clinical Research--Cooperative Agreements (U10)
Project #
5U10HL054497-03
Application #
2519500
Study Section
Special Emphasis Panel (ZHL1-CCT-M (F2))
Project Start
1995-09-05
Project End
2000-08-31
Budget Start
1997-09-01
Budget End
1998-08-31
Support Year
3
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Boston University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
604483045
City
Boston
State
MA
Country
United States
Zip Code
02118

  Publications

Wild, Philipp S; Felix, Janine F; Schillert, Arne et al. (2017) Large-scale genome-wide analysis identifies genetic variants associated with cardiac structure and function. J Clin Invest 127:1798-1812
Nandakumar, Priyanka; Lee, Dongwon; Richard, Melissa A et al. (2017) Rare coding variants associated with blood pressure variation in 15?914 individuals of African ancestry. J Hypertens 35:1381-1389
Selvaraj, Senthil; Djoussé, Luc; Aguilar, Frank G et al. (2017) Association of Estimated Sodium Intake With Adverse Cardiac Structure and Function: From the HyperGEN Study. J Am Coll Cardiol 70:715-724
Wang, Heming; Choi, Yoonha; Tayo, Bamidele et al. (2017) Genome-wide survey in African Americans demonstrates potential epistasis of fitness in the human genome. Genet Epidemiol 41:122-135
Taylor, Jacquelyn Y; Schwander, Karen; Kardia, Sharon L R et al. (2016) A Genome-wide study of blood pressure in African Americans accounting for gene-smoking interaction. Sci Rep 6:18812
Olfson, E; Saccone, N L; Johnson, E O et al. (2016) Rare, low frequency and common coding variants in CHRNA5 and their contribution to nicotine dependence in European and African Americans. Mol Psychiatry 21:601-7
Selvaraj, Senthil; Martinez, Eva E; Aguilar, Frank G et al. (2016) Association of Central Adiposity With Adverse Cardiac Mechanics: Findings From the Hypertension Genetic Epidemiology Network Study. Circ Cardiovasc Imaging 9:
Aguilar, Frank G; Selvaraj, Senthil; Martinez, Eva E et al. (2016) Archeological Echocardiography: Digitization and Speckle Tracking Analysis of Archival Echocardiograms in the HyperGEN Study. Echocardiography 33:386-97
Selvaraj, Senthil; Aguilar, Frank G; Martinez, Eva E et al. (2014) Diastolic wall strain: a simple marker of abnormal cardiac mechanics. Cardiovasc Ultrasound 12:40
Selvaraj, Senthil; Aguilar, Frank G; Martinez, Eva E et al. (2014) Association of comorbidity burden with abnormal cardiac mechanics: findings from the HyperGEN study. J Am Heart Assoc 3:e000631

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