Abstract

Histamine (HA), present in significant concentrations in cardiac mast cells (MC), is released immunologically or by ischemia-reperfusion (I/R), causing severe H2-receptor(H2R)-mediated tachyarrhythmias. These MC are in close proximity to sympathetic nerve terminals (SNT), which we have recently discovered to contain a different HA receptor subtype, H3R, that downregulates norepinephrine (NE) release. H3R quiescent, yet fully activated in hyperadrenergic states, such as myocardial ischemia, when HA is copiously released. We will test the hypothesis that H3R are also activated in the failing heart. Because cardiac MC are exposed to neuropeptides released from neighboring SNT (e.g., NPY) and sensory C- fibers (e.g., CGRP), we will investigate the influence of NPY and CGRP on cardiac HA release in normal and ischemic conditions. Further, we will directly investigate the transductional mechanisms associated with H3R- mediated inhibition of NE release in normal and ischemic SNT (synaptosomes) isolated from guinea pig hearts, from dogs in cardiac failure and from surgical specimens of human right atrium. Helped by pilot data, we postulate that H3R attenuate NE exocytosis (associated with acute ischemia) and """"""""carrier-mediated"""""""" release (associated with protracted ischemia and Na+/H+ antiporter activation), by inhibiting PI turnover and PKC activity. Indeed, we find that bradykinin (BK), which is known to stimulate the Na+/H+ exchanger, increases NE release associated with protracted ischemia. Accordingly, we propose to characterize the receptor subtype and transductional mechanisms mediating the BK-induced enhancement of NE release in protracted myocardial ischemia. Among other putative endogenous modulators of cardiac sympathetic neurotransmission, we plan to investigate in cardiac synaptosomes the effects of nitric oxide (NO), which we find to enhance or decrease NE exocytosis as a function of its concentration. We propose to determine the mechanisms mediating the facilitatory and inhibitory action of NO, focussing on whether NO facilitates NE release via a Ca2+-dependent or independent mechanism, and whether NO inhibits NE release by activating high-conductance Kca channels, thus hyperpolarizing SNT, and decreasing Ca2+ entry and exocytosis. Septic shock, the leading cause of death in intensive care units, is characterized by NO overproduction, depressed myocardial contractility and adrenergic derangement. In a septic shock model, we will determine whether the attending cardiac failure is associated with a decreased NE release reflecting the action of high NO concentrations on SNT. Collectively, the proposed studies will assess both the protective and deleterious effects of cardiac HA release and its modulation by multiple stimuli, as well as the transductional mechanisms involved in H3R signaling. The role of other endogenous modulators of SNT function (BK and NO) will be defined. Accordingly, the proposed studies will generate novel and significant information towards the development of new therapeutic strategies in cardiovascular diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL034215-25
Application #
6183640
Study Section
Pharmacology A Study Section (PHRA)
Project Start
1985-09-10
Project End
2001-08-31
Budget Start
2000-04-01
Budget End
2001-08-31
Support Year
25
Fiscal Year
2000
Total Cost
$438,143
Indirect Cost

  Institution

Name
Weill Medical College of Cornell University
Department
Pharmacology
Type
Schools of Medicine
DUNS #
201373169
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Marino, Alice; Sakamoto, Takuya; Robador, Pablo A et al. (2017) S1P receptor 1-Mediated Anti-Renin-Angiotensin System Cardioprotection: Pivotal Role of Mast Cell Aldehyde Dehydrogenase Type 2. J Pharmacol Exp Ther 362:230-242
Marino, Alice; Martelli, Alma; Citi, Valentina et al. (2016) The novel H2 S donor 4-carboxy-phenyl isothiocyanate inhibits mast cell degranulation and renin release by decreasing intracellular calcium. Br J Pharmacol 173:3222-3234
Aldi, Silvia; Marino, Alice; Tomita, Kengo et al. (2015) E-NTPDase1/CD39 modulates renin release from heart mast cells during ischemia/reperfusion: a novel cardioprotective role. FASEB J 29:61-9
Aldi, Silvia; Takano, Ken-ichi; Tomita, Kengo et al. (2014) Histamine H4-receptors inhibit mast cell renin release in ischemia/reperfusion via protein kinase C ?-dependent aldehyde dehydrogenase type-2 activation. J Pharmacol Exp Ther 349:508-17
Hu, Zhaoyang; Crump, Shawn M; Anand, Marie et al. (2014) Kcne3 deletion initiates extracardiac arrhythmogenesis in mice. FASEB J 28:935-45
Aldi, Silvia; Robador, Pablo A; Tomita, Kengo et al. (2014) IgE receptor-mediated mast-cell renin release. Am J Pathol 184:376-81
Chan, Noel Yan-Ki; Robador, Pablo A; Levi, Roberto (2012) Natriuretic peptide-induced catecholamine release from cardiac sympathetic neurons: inhibition by histamine H3 and H4 receptor activation. J Pharmacol Exp Ther 343:568-77
Robador, Pablo A; Seyedi, Nahid; Chan, Noel Yan-Ki et al. (2012) Aldehyde dehydrogenase type 2 activation by adenosine and histamine inhibits ischemic norepinephrine release in cardiac sympathetic neurons: mediation by protein kinase C?. J Pharmacol Exp Ther 343:97-105
Hashikawa-Hobara, Narumi; Chan, Noel Yan-Ki; Levi, Roberto (2012) Histamine 3 receptor activation reduces the expression of neuronal angiotensin II type 1 receptors in the heart. J Pharmacol Exp Ther 340:185-91
Chan, Noel Yan-Ki; Seyedi, Nahid; Takano, Kenichi et al. (2012) An unsuspected property of natriuretic peptides: promotion of calcium-dependent catecholamine release via protein kinase G-mediated phosphodiesterase type 3 inhibition. Circulation 125:298-307

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