Abstract

Investigations in the past decades have significantly advanced our understanding of signaling mechanisms underlying the protection and pathogenesis of myocardial ischemic injury. It is increasingly recognized that preservation of mitochondrial function plays a pivotal role in cardioprotection against ischemia reperfusion injury (I/R). However, it remains virtually unknown as to who the molecular targets of cardioprotection are in the mitochondria;what specific molecular events led to the protection of mitochondria;and whether there is a systems integration of cardioprotective signaling at the mitochondria to support the manifestation of a protected phenotype. Using a murine model of nitric oxide (NO) induced late phase of cardioprotection, we elect to examine the plausible intrinsic signaling properties of mitochondria using a novel experimental strategy enabling a parallel examination of mitochondrial signaling, mitochondrial proteomes, and mitochondrial behavior by computational modeling. The proposed studies are based upon preliminary evidence by others and our own demonstrating that activation of PKC?-Src module occurs in the NO donor treated mice and that both are localized to mitochondrial membranes. In this proposal we will test the innovative hypothesis that the PKC?-Src module interacts with the brief mPTP openings to protect cardiomyocytes from Ca++ overload induced jury. The working hypothesis is that NO activates PKC?-Src module, leading to brief mPTP openings which results in transients Ca++ releases and reactive oxygen species (ROS) bursts, and consequently inactivates Ca++ reuptake and further activates PKC?-Src to form a feed- forward loop. When the homeostasis is interrupted (e.g., calcium overload or elevated ROS), brief mPTP openings transits into irreversible, long-lasting mPTP openings, which instead induce cardiac injury. In this application we propose to delineate the functional effects of brief openings of mPTP on Ca++ handling and ROS production;and to elucidate mPTP regulation by the mitochondrial PKC?-Src module in the setting of NO-induced late phase of cardioprotection (Aim 1). In the specific Aim 2 we will conclusively establish the activation of a PKC?-Src signaling module in the mitochondria as a mandatory signaling element of NO-induced cardioprotection against myocardial ischemic injury. At last we will systematically define the molecular targets of mitochondrial Src-kinase in NO- induced late phase of cardioprotection (Aim 3). The proposed studies will advance our understanding of cardiac biology by providing novel mechanistic insights into how interactions of brief mPTP openings with mitochondrial PKC?-Src module can be beneficial in mediating NO-induced late phase of cardioprotection.

Public Health Relevance

It is increasingly recognized that preservation of mitochondrial function plays a pivotal role in cardioprotection against ischemia reperfusion injury despite unclear molecular mechanisms. The proposed studies aim to characterize a novel pathway whereby brief mitochondrial membrane transition may interact with PKC?-Src module to mediate NO-induced cardioprotection. Novel findings may lead to better understanding of cardiac pathobiology, which will eventually translate into better patient care.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL101228-02
Application #
8064425
Study Section
Special Emphasis Panel (ZHL1-CSR-N (F1))
Program Officer
Schwartz, Lisa
Project Start
2010-05-01
Project End
2014-02-28
Budget Start
2011-04-01
Budget End
2012-02-29
Support Year
2
Fiscal Year
2011
Total Cost
$685,195
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Physiology
Type
Schools of Medicine
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Korge, Paavo; Calmettes, Guillaume; John, Scott A et al. (2017) Reactive oxygen species production induced by pore opening in cardiac mitochondria: The role of complex III. J Biol Chem 292:9882-9895
Korge, Paavo; John, Scott A; Calmettes, Guillaume et al. (2017) Reactive oxygen species production induced by pore opening in cardiac mitochondria: The role of complex II. J Biol Chem 292:9896-9905
Korge, Paavo; Calmettes, Guillaume; Weiss, James N (2016) Reactive oxygen species production in cardiac mitochondria after complex I inhibition: Modulation by substrate-dependent regulation of the NADH/NAD(+) ratio. Free Radic Biol Med 96:22-33
Li, Qiang; Youn, Ji-Youn; Cai, Hua (2015) Mechanisms and consequences of endothelial nitric oxide synthase dysfunction in hypertension. J Hypertens 33:1128-36
Siu, Kin Lung; Lotz, Christopher; Ping, Peipei et al. (2015) Netrin-1 abrogates ischemia/reperfusion-induced cardiac mitochondrial dysfunction via nitric oxide-dependent attenuation of NOX4 activation and recoupling of NOS. J Mol Cell Cardiol 78:174-85
Korge, Paavo; Calmettes, Guillaume; Weiss, James N (2015) Increased reactive oxygen species production during reductive stress: The roles of mitochondrial glutathione and thioredoxin reductases. Biochim Biophys Acta 1847:514-25
Li, Qiang; Youn, Ji-Youn; Li, Shan et al. (2015) Reply: To PMID 25882860. J Hypertens 33:2368-70
Li, Qiang; Cai, Hua (2015) ANO1 taking center stage: blood pressure regulation in SHRs. J Mol Cell Cardiol 82:216-7
Ping, Peipei; Gustafsson, Åsa B; Bers, Don M et al. (2015) Harnessing the Power of Integrated Mitochondrial Biology and Physiology: A Special Report on the NHLBI Mitochondria in Heart Diseases Initiative. Circ Res 117:234-8
Youn, Ji Youn; Cai, Hua (2015) Fueling up skeletal muscle to reduce obesity: A TrkB story. Chem Biol 22:311-2

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