Abstract

Hypertension is a serious and prevalent disease. Current dogma states that the pathogenesis of hypertension requires abnormal renal sodium handling as the 'final common pathway'. The fundamental hypothesis being tested in this Program Project Grant (PPG) is that loss of the normal function of VSMC regulatory proteins can directly cause vascular diseases such as hypertension. We recently identified vascular dysfunction and associated hypertension in several genetically modified mice deficient in or expressing abnormal forms of VSMC contractile regulatory proteins. These mice lack gross abnormalities of renal function. Based on these observations we propose to test the hypothesis that hypertension can result from primary abnormalities of vascular smooth muscle cell function. Three of these hypertensive mouse lines will be studied in each of 3 specific aims: (1) protein kinase G Ialpha(PKGIalpha) leucine zipper mutant 'knock-in' (LZM KI) mice, which express a mutant PKGIalpha protein lacking a functional leucine zipper domain, (2) regulator of G protein signaling 2 knockout (RGS2KO) mice, and (3) estrogen receptor beta knockout (betaERKO) mice. We will explore the relationship between vascular dysfunction and hypertension in each of these mouse lines by examining the effects of transplantation of kidneys to and from the hypertensive mice and their wild type littermates, on blood pressure, vascular function, and renal function. For each gentotype, four groups of mice will studied: Group 1. hypertensive mice transplanted with a kidney from a hypertensive donor, Group 2. hypertensive mice transplanted with a kidney from a wild type littermate, Group 3. normotensive wild type mice transplanted with a kidney from another wild type mouse, and Group 4. wild type mice transplanted with a kidney from a hypertensive, genetically-altered mouse. Groups 1 and 3 will serve as controls for the transplant procedure, whereas comparison of the effects of transplantation on blood pressure, vascular function, and renal function in the mice in Groups 2 and 4 will reveal the relative contribution of the vascular dysfunction vs. any renal abnormalities to the hypertensive phenotype. Direct testing of our hypothesis, as proposed here, is of central importance to the conceptual framework upon which current approaches to the diagnosis and treatment of disorders of blood pressure are based. As such, these studies have the potential to advance our ability to diagnose and treat hypertension.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL077378-05
Application #
7673411
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Project Start
Project End
Budget Start
2008-08-01
Budget End
2009-07-31
Support Year
5
Fiscal Year
2008
Total Cost
$399,734
Indirect Cost

  Institution

Name
Tufts University
Department
Type
DUNS #
079532263
City
Boston
State
MA
Country
United States
Zip Code
02111

  Publications

Halder, Indrani; Matthews, Karen A; Buysse, Daniel J et al. (2015) African Genetic Ancestry is Associated with Sleep Depth in Older African Americans. Sleep 38:1185-93
Poh, Kian-Keong; Lu, Ping; Qin, Gangjian et al. (2013) Endothelial dysfunction and systemic hypertension by selective cGMP-dependent protein kinase I inhibition using novel cell-penetrating peptide delivered in vivo. Int J Cardiol 167:2114-9
Wang, Guang-rong; Surks, Howard K; Tang, K Mary et al. (2013) Steroid-sensitive gene 1 is a novel cyclic GMP-dependent protein kinase I substrate in vascular smooth muscle cells. J Biol Chem 288:24972-83
Blanton, Robert M; Takimoto, Eiki; Aronovitz, Mark et al. (2013) Mutation of the protein kinase I alpha leucine zipper domain produces hypertension and progressive left ventricular hypertrophy: a novel mouse model of age-dependent hypertensive heart disease. J Gerontol A Biol Sci Med Sci 68:1351-5
Wooten, Eric C; Hebl, Virginia B; Wolf, Matthew J et al. (2013) Formin homology 2 domain containing 3 variants associated with hypertrophic cardiomyopathy. Circ Cardiovasc Genet 6:10-8
Joshi, Shreena; Nelson, Mark T; Werner, Matthias E (2012) Amplified NO/cGMP-mediated relaxation and ryanodine receptor-to-BKCa channel signalling in corpus cavernosum smooth muscle from phospholamban knockout mice. Br J Pharmacol 165:455-66
Blanton, Robert M; Takimoto, Eiki; Lane, Angela M et al. (2012) Protein kinase g i? inhibits pressure overload-induced cardiac remodeling and is required for the cardioprotective effect of sildenafil in vivo. J Am Heart Assoc 1:e003731
Halder, Indrani; Kip, Kevin E; Mulukutla, Suresh R et al. (2012) Biogeographic ancestry, self-identified race, and admixture-phenotype associations in the Heart SCORE Study. Am J Epidemiol 176:146-55
Wooten, Eric C; Huggins, Gordon S (2011) Mind the dbGAP: the application of data mining to identify biological mechanisms. Mol Interv 11:95-102
Hill-Eubanks, David C; Werner, Matthias E; Heppner, Thomas J et al. (2011) Calcium signaling in smooth muscle. Cold Spring Harb Perspect Biol 3:a004549

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