Abstract

Energy metabolism enables cells to maintain an internal milieu different from that of the environment. It is no wonder, then, that eukaryotic cells have evolved mechanisms whereby changes in energy metabolism feed back upon and regulate ion transport. The applicant has recently discovered two such mechanisms in mammalian cardiac cells, where they may alter excitability and excitation-contraction coupling during ischemia. The first involves the regulation of L-type calcium channels. He has found that sudden jumps in intracellular MgATP (but not in either Mg2+ or ATP4- alone) up-regulate the calcium current in ventricular myocytes. This response is not dependent on phosphorylation: nonhydrolyzable ATP analogs support the response, and it remains robust even in the presence of protein kinase inhibitors. The evidence suggests a direct allosteric effect of MgATP on calcium channels. This application seeks to elucidate the biophysical and structural bases of this effect using electrophysiological and molecular genetic approaches. The second mechanism focuses on oscillations of membrane current and Ca2+ transients in which energy metabolism is the primary oscillator. The aplicant has found that heart cells subjected to moderate, reversible metabolic stress (for example, removal of external glucose) undergo spontaneous oscillations of membrane current. Large outward currents develop gradually, peak and subside with a period of one-two min; the currents are blocked by glibenclamide and suppressed by glucose. Although such oscillations are not initiated by intracellular Ca2+, depolarization-evoked Ca2+ transients are inhibited as the outward currents peak. Previous work in cardiac cystosolic extracts and in intact cells has demonstrated that glycolytic metabolites oscillate spontaneously, due to opposing feedback effects on the rate- limiting enzyme phosphofructokinase. In line with this idea, the investigator's preliminary data reveal that the membrane current oscillations can be initiated (or their phase reset) by sudden liberation of intracellular ADP or ATP using flash photolysis of caged compounds. The applicant will test the hypothesis that the membrane current is carried by ATP-dependent potassium channels driven by primary oscillations in the rate of glycolysis. Intracellular NADH and ATP concentrations will be measured to verify directly the presence of metabolic oscillations and to determine their magnitude. The investigator will also investigate the basis of the concomitant changes in excitation-contraction coupling. These two pathways by which metabolism can alter ionic currents merit investigation not only because of their novelty but also because of their potentially important contributions to arrhythmias and disorders of contractility.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37HL036957-12
Application #
2702174
Study Section
Cardiovascular and Renal Study Section (CVB)
Project Start
1986-07-01
Project End
2000-04-30
Budget Start
1998-05-01
Budget End
1999-04-30
Support Year
12
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Ardehali, Hossein; O'Rourke, Brian; Marban, Eduardo (2005) Cardioprotective role of the mitochondrial ATP-binding cassette protein 1. Circ Res 97:740-2
Ardehali, Hossein; Xue, Tian; Dong, Peihong et al. (2005) Targeting of the mitochondrial membrane proteins to the cell surface for functional studies. Biochem Biophys Res Commun 338:1143-51
Ardehali, Hossein; Chen, Zhenhui; Ko, Young et al. (2004) Multiprotein complex containing succinate dehydrogenase confers mitochondrial ATP-sensitive K+ channel activity. Proc Natl Acad Sci U S A 101:11880-5
Hsu, Kate; Seharaseyon, Jegatheesan; Dong, Peihong et al. (2004) Mutual functional destruction of HIV-1 Vpu and host TASK-1 channel. Mol Cell 14:259-67
Murata, Mitsushige; Cingolani, Eugenio; McDonald, Amy D et al. (2004) Creation of a genetic calcium channel blocker by targeted gem gene transfer in the heart. Circ Res 95:398-405
Teshima, Yasushi; Akao, Masaharu; Baumgartner, William A et al. (2003) Nicorandil prevents oxidative stress-induced apoptosis in neurons by activating mitochondrial ATP-sensitive potassium channels. Brain Res 990:45-50
Teshima, Yasushi; Akao, Masaharu; Li, Ronald A et al. (2003) Mitochondrial ATP-sensitive potassium channel activation protects cerebellar granule neurons from apoptosis induced by oxidative stress. Stroke 34:1796-802
Teshima, Yasushi; Akao, Masaharu; Jones, Steven P et al. (2003) Uncoupling protein-2 overexpression inhibits mitochondrial death pathway in cardiomyocytes. Circ Res 93:192-200
Akao, Masaharu; O'Rourke, Brian; Teshima, Yasushi et al. (2003) Mechanistically distinct steps in the mitochondrial death pathway triggered by oxidative stress in cardiac myocytes. Circ Res 92:186-94
Akao, Masaharu; O'Rourke, Brian; Kusuoka, Hideo et al. (2003) Differential actions of cardioprotective agents on the mitochondrial death pathway. Circ Res 92:195-202

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