The link between salt-sensitivity/dietary sodium and the development of high blood pressure is widely accepted. However, in spite of the extensive research that has been done in this area, the specific mechanism(s) involved in salt-induced hypertension remain unclear. The long-term goal of this research project is to examine the hypothesis that dietary salt increased blood pressure by modifying vascular reactivity, in part, via enhancement of sympathetic activity and suppression of nitric oxide activity/function.
The specific aims are: 1) Examine the mechanism(s) involved in the pathogenesis of salt-induced hypertension with emphasis on cardiovascular, hemodynamics and vascular reactivity, in male and female, conscious and pithed Dahl salt-sensitive and salt-resistant rats. 2) Elucidate the signal transduction pathways and ion channels involved in salt-induced hypertension by nitric oxide, cyclic GMP, neurotransmitter release and Ca/2+ in the isolated aorta. Blood pressure and heart rate will be measured indirectly by tail plethysmography as well as directly in conscious rats. Cardiac output and stroke volume will be measured using a Cardiomax II and total peripheral resistance calculated. Vascular reactivity to sodium nitroprusside, phenylephrine and norepinephrine as influence by -adrenoceptors and sympathetic stimulation as well as the effect of Ca/2+ channel blocker will be evaluated in both conscious and pithed rats. Blood flow to discrete vascular beds (aortic, mesenteric and renal) will be determined using a Transonic flow-meter. Blood samples will be collected from arterial catheters implanted in the femoral arteries. Plasma levels of catecholamine and cGMP will be assayed by high performance liquid chromatography with electrochemical detection and radio-immunoassay, respectively. Cyclic AMP and cGMP levels and intracellular Ca/2+ will also be measure din isolated rat aorta endothelial cells. Data derived from these studies will provide new insights related to gender differences and cardiovascular and cellular mechanism(s) involved in salt-induced hypertension.

Project Start
1998-08-01
Project End
1999-07-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
12
Fiscal Year
1998
Total Cost
Indirect Cost
Name
Morehouse School of Medicine
Department
Type
DUNS #
City
Atlanta
State
GA
Country
United States
Zip Code
30310
Wilson, Nana; Driss, Adel; Solomon, Wesley et al. (2013) CXCL10 gene promoter polymorphism -1447A>G correlates with plasma CXCL10 levels and is associated with male susceptibility to cerebral malaria. PLoS One 8:e81329
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Wilson, Nana O; Solomon, Wesley; Anderson, Leonard et al. (2013) Pharmacologic inhibition of CXCL10 in combination with anti-malarial therapy eliminates mortality associated with murine model of cerebral malaria. PLoS One 8:e60898
Igietseme, Joseph U; Omosun, Yusuf; Partin, James et al. (2013) Prevention of Chlamydia-induced infertility by inhibition of local caspase activity. J Infect Dis 207:1095-104
Shelton, Martin N; Huang, Ming-Bo; Ali, Syed A et al. (2012) Secretion modification region-derived peptide disrupts HIV-1 Nef's interaction with mortalin and blocks virus and Nef exosome release. J Virol 86:406-19
Campbell, Patrick E; Isayev, Olexandr; Ali, Syed A et al. (2012) Validation of a novel secretion modification region (SMR) of HIV-1 Nef using cohort sequence analysis and molecular modeling. J Mol Model 18:4603-13
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Wilson, Nana O; Ceesay, Fatou K; Obed, Samuel A et al. (2011) Intermittent preventive treatment with sulfadoxine-pyrimethamine against malaria and anemia in pregnant women. Am J Trop Med Hyg 85:12-21
Lucchi, Naomi W; Jain, Vidhan; Wilson, Nana O et al. (2011) Potential serological biomarkers of cerebral malaria. Dis Markers 31:327-35

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