Abstract

The propose research in project 5 is based on two working hypotheses: (a) spinal nicotinic cholinergic neurotransmission is a critical pathway in the maintenance of blood pressure and in mediating pressor responses elicited by external stimulae; (b) certain hypertensive phenotypes with a genetic basis result from hyper-excitability of the nicotinic system which amplifies responses to central stimulation through control by presynaptic receptors. Thus, hypertension and enhanced startle responses may be critical manifestations of hyper-excitability spinal nicotinic receptor regulated pathways. In the past award period we have mapped some of the critical pathways involved in the spinal pressor response, described differential responses to nicotinic agonists and examined amino acid release and nicotinic receptor densities in spontaneously hypertensive rat (SHR) and control (WKY) rats. We plan to extend these studies to recombinant inbred strains and to hypertension models that do not have a primary, central neurogenic component in order to determine whether nicotinic hyperexcitability cosegregates with hypertension and whether it is confined to neurogenic hypertension with a genetic origin. Recently, we developed an intrathecal microdialysis system that enables injection of nicotinic agonists and measurement of released neurotransmitters into the intrathecal space in apposition to the injection site. This cellular endpoint of neurotransmitter release will be correlated with radioligand detection of receptors by autoradiography in spinal sections and with the pharmacologic endpoints. These techniques will enable us to extend our analysis to the cellular and molecular levels. These studies will initially be directed to completing our analysis of nicotinic agonist mediated release of excitatory amino acids and then extending the studies to release of acetylcholine, substance P and catecholamines. We propose to identify cellular mediators such as intracellular Ca2+ and regulators of gene expression that may be responsible for the enhanced excitability of the spinal responses. These studies will interface with Projects 1 and 2. Specific procedures for ablation of primary afferents, ascending and descending pathways and interneurons have been developed and the influence of these interventions will be examined on the responses in the intact animal, the cellular response of transmitter release and the loss of nicotinic receptor subtypes and their localization. Second, we will examine the specificity and subtypes of nicotinic receptors involved through the use of receptor selective ligands, immunoprecipitation, and autoradiography and plan to correlate this information with the loci of genes affecting hypertension. Third, receptor subtype expression in the spinal cord will be correlated with the mRNA species through message protection and in situ hybridization.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
2P01HL035018-12
Application #
6272744
Study Section
Project Start
1998-07-01
Project End
1999-06-30
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
12
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of California San Diego
Department
Type
DUNS #
077758407
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Harrall, Kylie K; Kechris, Katerina J; Tabakoff, Boris et al. (2016) Uncovering the liver's role in immunity through RNA co-expression networks. Mamm Genome 27:469-84
Saba, Laura M; Flink, Stephen C; Vanderlinden, Lauren A et al. (2015) The sequenced rat brain transcriptome--its use in identifying networks predisposing alcohol consumption. FEBS J 282:3556-78
Vanderlinden, Lauren A; Saba, Laura M; Printz, Morton P et al. (2014) Is the alcohol deprivation effect genetically mediated? Studies with HXB/BXH recombinant inbred rat strains. Alcohol Clin Exp Res 38:2148-57
Pravenec, Michal; Kozich, Viktor; Krijt, Jakub et al. (2013) Folate deficiency is associated with oxidative stress, increased blood pressure, and insulin resistance in spontaneously hypertensive rats. Am J Hypertens 26:135-40
Necká?, Jan; Šilhavy, Jan; Zídek, Václav et al. (2012) CD36 overexpression predisposes to arrhythmias but reduces infarct size in spontaneously hypertensive rats: gene expression profile analysis. Physiol Genomics 44:173-82
Houstek, Josef; Hejzlarova, Katerina; Vrbacky, Marek et al. (2012) Nonsynonymous variants in mt-Nd2, mt-Nd4, and mt-Nd5 are linked to effects on oxidative phosphorylation and insulin sensitivity in rat conplastic strains. Physiol Genomics 44:487-94
Pravenec, Michal; Zidek, Vaclav; Landa, Vladimir et al. (2011) Age-related autocrine diabetogenic effects of transgenic resistin in spontaneously hypertensive rats: gene expression profile analysis. Physiol Genomics 43:372-9
Wikoff, William R; Nagle, Megha A; Kouznetsova, Valentina L et al. (2011) Untargeted metabolomics identifies enterobiome metabolites and putative uremic toxins as substrates of organic anion transporter 1 (Oat1). J Proteome Res 10:2842-51
Malínská, Hana; Oliyarnyk, Olena; Hubová, Miriam et al. (2010) Increased liver oxidative stress and altered PUFA metabolism precede development of non-alcoholic steatohepatitis in SREBP-1a transgenic spontaneously hypertensive rats with genetic predisposition to hepatic steatosis. Mol Cell Biochem 335:119-25
Rosines, Eran; Johkura, Kohei; Zhang, Xing et al. (2010) Constructing kidney-like tissues from cells based on programs for organ development: toward a method of in vitro tissue engineering of the kidney. Tissue Eng Part A 16:2441-55

Showing the most recent 10 out of 187 publications