Abstract

Factors that accumulate with age such as increased sodium intake have been linked to age-associated vascular dysfunction, increased blood pressure and the onset of cardiovascular diseases. However, the mechanisms that mediate interaction between environmental factors such as dietary salt intake and an individual's genetic background resulting in age-associated blood pressure increases are unclear. This supplemental application is a Revision to a recently funded proposal focused on the characterization of a newly identified association between striatin, a caveolin-1 binding protein, and two factors: aldosterone (ALDO)'s mechanisms of action and vascular function. We have recently documented that striatin is a key intermediate in: 1) ALDO's non-genomic mechanism of action; 2) the blood pressure response to sodium intake in humans and mice; and 3) . polymorphic variants of the striatin gene are associated with salt sensitive hypertension in humans. Also, our Preliminary Results show that 1) young male striatin heterozygous knockout mice (STRN+/-) have increased Na+ sensitive blood pressure and altered vascular vasodilator responses that are associated with reduced striatin levels; 2) but, young female STRN+/- mice do not appear to have Na+ sensitive blood pressure even though they have reduced striatin levels. 3) However, female STRN+/- but not female wild type (WT) mice have an age-related trend to Na+ sensitive blood pressure. These data suggest that striatin: 1) is a novel key modulator of ALDO's mechanisms of action; 2) is likely an important modulator of vascular function; and 3) variation in striatin gene expression may in part mediate vascular responses to changes in salt intake that are likely potentiated by aging. Consequently, as age and high dietary salt intake are predictors of hypertension, we hypothesize that striatin modulates the interaction of age and salt intake on blood pressure. These novel findings provide entre to this proposal that focuses on studying aged mice in order to conduct age-based analyses. Our goals will be assessed through the following Aim: 1) To test the hypothesis that in mice, age and striatin interact to modify aldosterone and vascular responses to changes in Na+ intake. These novel studies will take advantage our recently characterized mouse model of reduced striatin levels to perform three series of studies in 18 month old mice and 1) characterize the blood pressure responses to Na+ intake in STRN+/- male and female mice; 2) isolate the aortas from these mice and characterize the effects of aortic responses to acetylcholine and phenylephrine; and 3) study primary aortic endothelial cells isolated from these mice to characterize the direct effects of ALDO in these cells. These studies are significant as they will address how striatin may modify aging and aging-related processes that affect the progression of a chronic disorder such as hypertension.

Public Health Relevance

Striatin is a protein that interacts with important receptors within cells that regulate the function of the heart and blood vessels. Striatin deficiency impairs the ability of vessels to respond appropriately to steroids like aldosterone and estrogen. This project will assess the role of aging on the mechanisms by which striatin and dietary salt can lead to changes in blood pressure and blood vessel function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
3R01HL114765-03S1
Application #
8961416
Study Section
Special Emphasis Panel (ZHL1-CSR-P (M3))
Program Officer
Mcdonald, Cheryl
Project Start
2012-07-01
Project End
2017-06-30
Budget Start
2015-09-14
Budget End
2016-06-30
Support Year
3
Fiscal Year
2015
Total Cost
$126,773
Indirect Cost
$51,773

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
030811269
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Gupta, Tina; Connors, Molly; Tan, Jia Wei et al. (2017) Striatin Gene Polymorphic Variants Are Associated With Salt Sensitive Blood Pressure in Normotensives and Hypertensives. Am J Hypertens 31:124-131
Hundemer, Gregory L; Baudrand, Rene; Brown, Jenifer M et al. (2017) Renin Phenotypes Characterize Vascular Disease, Autonomous Aldosteronism, and Mineralocorticoid Receptor Activity. J Clin Endocrinol Metab 102:1835-1843
Chong, Cherish; Hamid, Anis; Yao, Tham et al. (2017) Regulation of aldosterone secretion by mineralocorticoid receptor-mediated signaling. J Endocrinol 232:525-534
Garza, Amanda E; Pojoga, Luminita H; Moize, Burhanuddin et al. (2015) Critical Role of Striatin in Blood Pressure and Vascular Responses to Dietary Sodium Intake. Hypertension 66:674-80
Baudrand, Rene; Pojoga, Luminita H; Vaidya, Anand et al. (2015) Statin Use and Adrenal Aldosterone Production in Hypertensive and Diabetic Subjects. Circulation 132:1825-33
Pojoga, Luminita H; Yao, Tham M; Opsasnick, Lauren A et al. (2015) Cooperative Role of Mineralocorticoid Receptor and Caveolin-1 in Regulating the Vascular Response to Low Nitric Oxide-High Angiotensin II-Induced Cardiovascular Injury. J Pharmacol Exp Ther 355:32-47
Garza, Amanda E; Rariy, Chevon M; Sun, Bei et al. (2015) Variants in striatin gene are associated with salt-sensitive blood pressure in mice and humans. Hypertension 65:211-217
Baudrand, R; Lian, C G; Lian, B Q et al. (2014) Long-term dietary sodium restriction increases adiponectin expression and ameliorates the proinflammatory adipokine profile in obesity. Nutr Metab Cardiovasc Dis 24:34-41
Coutinho, Patricia; Vega, Christopher; Pojoga, Luminita H et al. (2014) Aldosterone's rapid, nongenomic effects are mediated by striatin: a modulator of aldosterone's effect on estrogen action. Endocrinology 155:2233-43
Baudrand, Rene; Pojoga, Luminita H; Romero, Jose R et al. (2014) Aldosterone's mechanism of action: roles of lysine-specific demethylase 1, caveolin and striatin. Curr Opin Nephrol Hypertens 23:32-7

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