Abstract

Two central hypotheses will be explored: 1) Enhanced peripheral chemoreflex function contributes to the development and maintenance of impaired baroreflex function and elevated resting sympathetic function in the rabbit model of pacing-induced heart failure (HF); and 2) Down-regulation of nitric oxide synthase (NOS) in the carotid body (CB) during the development of HF leads to altered ion channel function of type I cells and enhanced CB chemoreceptor sensitivity. To test the first hypothesis, we will determine the time-course of changes in peripheral chemoreflex and baroreflex control of renal sympathetic nerve activity and ventilation during the development of HF in conscious rabbits; and to determine whether the altered peripheral chemoreflex function contributes to impaired baroreflex function and the elevation in resting sympathetic activity in the HF state. To test the second hypothesis, we will determine whether NOS contributes to the altered discharge characteristics or CB chemoreceptor afferents in HF rabbits in response to graded levels of hypoxia, hypercapnia, and chemical stimuli. Afferent responses to these stimuli will be assessed before and after NOS inhibition, exposure to an NO donor to 1 arginine. In other experiments, afferent responses to stimuli will be assessed before and after guanylate cyclase inhibition, phosphodiesterase inhibition, or exposure to cGMP analogues to determine the extent to which NO effects can be attributed to cGMP activation. Using a whole cell patch-clamp, we will determine whether the current density of O2-sensitive K+ channels is altered in CB type 1 (glomus) cells of HF rabbits, and determine whether NOS and cGMP pathways contribute to the altered K+ channel characteristics of these type I cells as in the afferent experiments. We will determine the extent to which NOS activity and the expression and distribution of endothelial (ec) and neural (nc) NOS in cells within the CB is altered in HF rabbits. We will: measure expression of ec- and nc-NOS mRNA in the CB using RT-PCR methods; measure the distribution of NOS isoforms in the CB using immunocytochemical methods; and measure NO production from Cbs under normoxic and graded hypoxic conditions using enzymatic and chemiluminescence methods.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL062222-02
Application #
6324753
Study Section
Project Start
2000-07-01
Project End
2001-06-30
Budget Start
Budget End
Support Year
2
Fiscal Year
2000
Total Cost
$153,201
Indirect Cost

  Institution

Name
University of Nebraska Medical Center
Department
Type
DUNS #
City
Omaha
State
NE
Country
United States
Zip Code
68198

  Publications

Tian, Changhai; Gao, Lie; Zimmerman, Matthew C et al. (2018) Myocardial infarction-induced microRNA-enriched exosomes contribute to cardiac Nrf2 dysregulation in chronic heart failure. Am J Physiol Heart Circ Physiol 314:H928-H939
Marcus, Noah J; Del Rio, Rodrigo; Ding, Yanfeng et al. (2018) KLF2 mediates enhanced chemoreflex sensitivity, disordered breathing and autonomic dysregulation in heart failure. J Physiol 596:3171-3185
Fontes, Marco Antônio Peliky; Vaz, Gisele Cristiane; Cardoso, Thais Zielke Dias et al. (2018) GABA-containing liposomes: neuroscience applications and translational perspectives for targeting neurological diseases. Nanomedicine 14:781-788
de Morais, Sharon D B; Shanks, Julia; Zucker, Irving H (2018) Integrative Physiological Aspects of Brain RAS in Hypertension. Curr Hypertens Rep 20:10
Zheng, Hong; Katsurada, Kenichi; Liu, Xuefei et al. (2018) Specific Afferent Renal Denervation Prevents Reduction in Neuronal Nitric Oxide Synthase Within the Paraventricular Nucleus in Rats With Chronic Heart Failure. Hypertension 72:667-675
Lewis, Robert; Hackfort, Bryan T; Schultz, Harold D (2018) Chronic Heart Failure Abolishes Circadian Rhythms in Resting and Chemoreflex Breathing. Adv Exp Med Biol 1071:129-136
Schiller, Alicia M; Pellegrino, Peter Ricci; Zucker, Irving H (2017) Eppur Si Muove: The dynamic nature of physiological control of renal blood flow by the renal sympathetic nerves. Auton Neurosci 204:17-24
Del Rio, Rodrigo; Andrade, David C; Toledo, Camilo et al. (2017) Carotid Body-Mediated Chemoreflex Drive in The Setting of low and High Output Heart Failure. Sci Rep 7:8035
Becker, Bryan K; Wang, Hanjun; Zucker, Irving H (2017) Central TrkB blockade attenuates ICV angiotensin II-hypertension and sympathetic nerve activity in male Sprague-Dawley rats. Auton Neurosci 205:77-86
Zheng, Hong; Liu, Xuefei; Li, Yulong et al. (2017) A Hypothalamic Leptin-Glutamate Interaction in the Regulation of Sympathetic Nerve Activity. Neural Plast 2017:2361675

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