Abstract

Hypertension is a complex disorder whose expression is determined by numerous genetic as well as environmental factors. The problem of identifying the genes involved is complex. Studies of hypertension in human subjects are complicated by non-Mendelian inheritance, genetic heterogeneity, a late age of onset, incomplete penetrance, and environmental influences. However, recent advances, including the increased ability to delineate the disordered physiology related to hypertension, the discovery of highly polymorphic molecular genetic markers, the development of new strategies for analysis of complex genetic disorders, the development of the relevant statistical programs, and the ready availability of much faster computers, have put the identification of genes making even relatively modest contributions to the disease within reach. The goal of Project 2 is to identify specific genes and regions within the human genome contributing to blood pressure regulation and intermediate hypertension phenotypes, with particular emphasis on insulin resistance and salt sensitivity. We will search for genetic loci by systematically mapping the entire human genome using highly polymorphic molecular markers in approximately 200 extensively phenotyped Mexican American families with over 600 sibpairs. These families will be ascertained via a proband with hypertension. A systematic mapping approach is particularly appropriate since there are so many potential candidate genes for blood pressure regulation. Although an alternative approach would be to first study all of these candidate genes, the methodology necessary for directly studying candidate genes (ie RFLP analysis, frequently requiring Southern blotting) is costly and inefficient. We therefore propose to begin with a systematic mapping approach, followed by targeted study of only those candidate genes that map within regions of interest identified by the systematic mapping. Once candidate gene regions are identified by systematic mapping, more detailed linkage analyses of specific candidate genes within these regions, as well as fine mapping of regions without known candidate genes, will be undertaken.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Specialized Center (P50)
Project #
1P50HL055005-01
Application #
5214369
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Baudrand, Rene; Goodarzi, Mark O; Vaidya, Anand et al. (2015) A prevalent caveolin-1 gene variant is associated with the metabolic syndrome in Caucasians and Hispanics. Metabolism 64:1674-81
Goodarzi, M O; Guo, X; Cui, J et al. (2013) Systematic evaluation of validated type 2 diabetes and glycaemic trait loci for association with insulin clearance. Diabetologia 56:1282-90
Guo, X; Cui, J; Jones, M R et al. (2012) Insulin clearance: confirmation as a highly heritable trait, and genome-wide linkage analysis. Diabetologia 55:2183-92
Williams, Jonathan S; Chamarthi, Bindu; Goodarzi, Mark O et al. (2012) Lysine-specific demethylase 1: an epigenetic regulator of salt-sensitive hypertension. Am J Hypertens 25:812-7
Pojoga, Luminita H; Underwood, Patricia C; Goodarzi, Mark O et al. (2011) Variants of the caveolin-1 gene: a translational investigation linking insulin resistance and hypertension. J Clin Endocrinol Metab 96:E1288-92
Goodarzi, Mark O; Taylor, Kent D; Jones, Michelle R et al. (2009) Replication of calpain-10 genetic association with carotid intima-media thickness. Atherosclerosis 205:503-5
Kopf, Daniel; Cheng, Li S-C; Blandau, Petra et al. (2008) Association of insulin sensitivity and glucose tolerance with the c.825C>T variant of the G protein beta-3 subunit gene. J Diabetes Complications 22:205-9
Xiang, Anny H; Azen, Stanley P; Buchanan, Thomas A et al. (2002) Heritability of subclinical atherosclerosis in Latino families ascertained through a hypertensive parent. Arterioscler Thromb Vasc Biol 22:843-8
Bosken, C H; Ko, Y C; Shete, S et al. (2001) Adaptations of linkage and association methods for the study of asthma, a complex trait. Genet Epidemiol 21 Suppl 1:S89-96
Cheng, L S; Davis, R C; Raffel, L J et al. (2001) Coincident linkage of fasting plasma insulin and blood pressure to chromosome 7q in hypertensive hispanic families. Circulation 104:1255-60

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