Abstract

The goal of this research is to elucidate the critical cellular changes that lead to irreversible cell injury. These mechanisms must be understood before rational interventions can be proposed. Previously, we have shown that an increase in cytosolic free calcium is associated with cell injury. In many systems, it has been observed that exposure of cells or animals to a brief stress provides considerable protection against a subsequent more severe stress. This brief period of stress is known to result in the synthesis of stress proteins; however, in spite of the identification of these proteins, there is little understanding of the mechanisms of protection. Exposing perfused rat heart to several brief (5 minute) periods of anoxic stress (referred to as preconditioning) affords protection when these preconditioned hearts are subjected to a longer 30-60 minute period of anoxic stress such that the preconditioned hearts have less necrosis and better recovery of function compared to untreated controls. Using 31P nuclear magnetic resonance(NMR) we have determined that preconditioning decreased the rate of ATP utilization; preconditioned hearts have a slower rate of decline in ATP and a reduced rate of anaerobic glycolysis. In addition, using a combination of 31P NMR and 19F NMR (to measure intracellular calcium) we have determined that the reduced metabolism results in less H+ production, and therefore less Na/H and Na/Ca exchange and ultimately less of an increase in cytosolic free calcium. We conclude that at least part of the protective effect of preconditioning is due to reduced calcium overload. We were interested in addressing the mechanism(s) responsible for the reduced rate of ATP utilization. We have investigated the hypothesis that adenosine is the mediator of preconditioning; however, in perfused rat heart adenosine does not appear to play such a role since we were unable to block the effect with an adenosine antagonist. In addition, we were not able to block preconditioning by the addition of glibenclamide, thus ruling out a role for the ATP sensitive K channels as part of this process.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Intramural Research (Z01)
Project #
1Z01ES010004-13
Application #
3840980
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
13
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
National Institute of Environmental Health Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Huss, Janice M; Imahashi, Ken-ichi; Dufour, Catherine R et al. (2007) The nuclear receptor ERRalpha is required for the bioenergetic and functional adaptation to cardiac pressure overload. Cell Metab 6:25-37
Delozier, Tracy C; Kissling, Grace E; Coulter, Sherry J et al. (2007) Detection of human CYP2C8, CYP2C9, and CYP2J2 in cardiovascular tissues. Drug Metab Dispos 35:682-8
Murphy, Elizabeth; Steenbergen, Charles (2007) Cardioprotection in females: a role for nitric oxide and altered gene expression. Heart Fail Rev 12:293-300
Murphy, Elizabeth; Steenbergen, Charles (2007) Gender-based differences in mechanisms of protection in myocardial ischemia-reperfusion injury. Cardiovasc Res 75:478-86
Murphy, Elizabeth; Steenbergen, Charles (2007) Preconditioning: the mitochondrial connection. Annu Rev Physiol 69:51-67
Nikolic, Ivana; Liu, Dianxin; Bell, Jamie A et al. (2007) Treatment with an estrogen receptor-beta-selective agonist is cardioprotective. J Mol Cell Cardiol 42:769-80
Shiva, Sruti; Huang, Zhi; Grubina, Rozalina et al. (2007) Deoxymyoglobin is a nitrite reductase that generates nitric oxide and regulates mitochondrial respiration. Circ Res 100:654-61
Sun, Junhui; Picht, Eckard; Ginsburg, Kenneth S et al. (2006) Hypercontractile female hearts exhibit increased S-nitrosylation of the L-type Ca2+ channel alpha1 subunit and reduced ischemia/reperfusion injury. Circ Res 98:403-11
Sun, Junhui; Steenbergen, Charles; Murphy, Elizabeth (2006) S-nitrosylation: NO-related redox signaling to protect against oxidative stress. Antioxid Redox Signal 8:1693-705
Seubert, John M; Sinal, Christopher J; Graves, Joan et al. (2006) Role of soluble epoxide hydrolase in postischemic recovery of heart contractile function. Circ Res 99:442-50

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