Abstract

The overall goal of Project by Jose is to determine D3, D1, and AT1 receptor interaction in the kidney. The D3 dopamine receptor can regulate renal sodium transport and blood pressure independent of the D1 receptor because disruption of the D3 receptor in mice increases blood pressure and impairs their ability to excrete an acute saline load. However, the D3 receptor can also synergistically interact with the D1 receptor to increase sodium excretion. In rodent models of genetic hypertension (Dahl salt sensitive and spontaneously hypertensive rat, SHR), the natriuretic effect of D3 receptors is impaired and the interaction between the D1 and D3 receptor is lost. The impairment of the renal D1 receptor function in genetic hypertension is caused by increased activity of G protein-coupled receptor kinase, type 4 (GRK4). GRK4 gene locus is linked to and GRK4 variants are associated with human essential hypertension. Heterologous expression of these variants in Chinese hamster ovary and HEK cells impairs D1 receptor function and mice overexpressing the GRK4 variant A142V develop hypertension and have an impaired natriuretic response to D1 receptor agonist stimulation. Moreover, inhibition of GRK4 activity in renal proximal tubule cells (or cell lines) from human hypertensives restores D1 receptor function and selective renal inhibition of GRK4 expression attenuates the increase in blood pressure in SHRs. Whether the impaired renal D3 receptor function in genetic hypertension is secondary to increased GRK4 activity, which impairs both the D1 and D3 receptor, is not known. However, D3-/- mice have impaired D1 receptor function, and increased renal renin content and AT1 receptor. Thus, a decreased D1 receptor and an increased AT1 receptor function in D3-/- mice may contribute to their impaired ability to excrete a saline load and hypertension. The overall hypothesis of Project by Jose is that renal proximal tubule sodium transport is regulated, in part, by an interaction among D1, D3 and AT1 receptors, acutely, by receptor/receptor interaction, and chronically, by regulation of receptor expression. Moreover, in genetic hypertension, impaired D3 (and D1) receptor function due to increased GRK4 activity, allows unimpeded AT1 receptor action.
Specific aim I will test the hypothesis that D3 receptor deficiency in mice both impairs D1 receptor function and allows unimpeded AT1 receptor function.
Specific aim 2 will test the hypothesis that increased GRK4 activity, due to constitutively active variants, impairs D3 receptor function in genetic hypertension. The results of these studies, using molecular biological and pharmacological tools, may shed light into the possibility that ability of GRK4 to regulate several genes may make GRK4 dysfunction a major cause of genetic hypertension.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
1P01HL074940-01
Application #
6781667
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Project Start
2003-12-01
Project End
2008-11-30
Budget Start
2003-12-01
Budget End
2005-03-31
Support Year
1
Fiscal Year
2004
Total Cost
$563,644
Indirect Cost

  Institution

Name
University of Virginia
Department
Type
DUNS #
065391526
City
Charlottesville
State
VA
Country
United States
Zip Code
22904

  Publications

Muntner, Paul; Whelton, Paul K; Woodward, Mark et al. (2018) A Comparison of the 2017 American College of Cardiology/American Heart Association Blood Pressure Guideline and the 2017 American Diabetes Association Diabetes and Hypertension Position Statement for U.S. Adults With Diabetes. Diabetes Care 41:2322-2329
Ye, Zhengmeng; Lu, Xi; Deng, Yi et al. (2018) In Utero Exposure to Fine Particulate Matter Causes Hypertension Due to Impaired Renal Dopamine D1 Receptor in Offspring. Cell Physiol Biochem 46:148-159
Yang, Yang; Chen, Caiyu; Fu, Chunjiang et al. (2018) Angiotensin II type 2 receptor inhibits expression and function of insulin receptor in rat renal proximal tubule cells. J Am Soc Hypertens 12:135-145
Li, Fengmin; Yang, Jian; Villar, Van Anthony M et al. (2018) Loss of renal SNX5 results in impaired IDE activity and insulin resistance in mice. Diabetologia 61:727-737
Wang, Xiaoyan; Villar, Van Anthony; Tiu, Andrew et al. (2018) Dopamine D2 receptor upregulates leptin and IL-6 in adipocytes. J Lipid Res 59:607-614
Luo, Hao; Chen, Caiyu; Guo, Li et al. (2018) Exposure to Maternal Diabetes Mellitus Causes Renal Dopamine D1 Receptor Dysfunction and Hypertension in Adult Rat Offspring. Hypertension 72:962-970
Wu, Gengze; Jose, Pedro A; Zeng, Chunyu (2018) Noncoding RNAs in the Regulatory Network of Hypertension. Hypertension 72:1047-1059
Asico, Laureano D; Cuevas, Santiago; Ma, Xiaobo et al. (2018) Nephron segment-specific gene expression using AAV vectors. Biochem Biophys Res Commun 497:19-24
Tiu, Andrew C; Bishop, Michael D; Asico, Laureano D et al. (2017) Primary Pediatric Hypertension: Current Understanding and Emerging Concepts. Curr Hypertens Rep 19:70
Diao, Zhenyu; Asico, Laureano D; Villar, Van Anthony M et al. (2017) Increased renal oxidative stress in salt-sensitive human GRK4?486V transgenic mice. Free Radic Biol Med 106:80-90

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