Cariporide preserves mitochondrial proton gradient and delays ATP  depletion in cardiomyocytes during ischemic conditions

Ruiz‐Meana, Marisol; Garcı́a-Dorado, David; Pina, Pilar; Inserte, Javier; Agulló, Luís; Soler‐Soler, Jordi

doi:10.1152/ajpheart.00035.2003

Cited by 88 publications

(62 citation statements)

References 32 publications

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“…In the present study, we used cationic lipophilic probe JC-1 (32)(33)(34) to assess the mitochondrial membrane potential (⌬ m ). In this assay, the mitochondria of nonapoptotic cells appeared in red following the aggregation of the JC-1 reagent, which emits red fluorescence at 590 nm (Fig.…”

Section: Resultsmentioning

confidence: 99%

Phosphodiesterase-5 Inhibitor Sildenafil Preconditions Adult Cardiac Myocytes against Necrosis and Apoptosis

Das

Xi²,

Kukreja

2005

Journal of Biological Chemistry

320

276

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We investigated the effect of sildenafil in protection against necrosis or apoptosis in cardiomyocytes. Adult mouse ventricular myocytes were treated with sildenafil (1 or 10 M) for 1 h before 40 min of simulated ischemia (SI). Necrosis was determined by trypan blue exclusion and lactate dehydrogenase release following SI alone or plus 1 or 18 h of reoxygenation (RO). Apoptosis was assessed by terminal deoxynucleotidyl transferase-mediated nick end labeling assay and mitochondrial membrane potential measured using a fluorescent probe 5,5 ,6,6 -tetrachloro-1,1 ,3,3 -tetraethylbenzimidazolyl-carbocyanine iodide (JC-1). Sildenafil reduced necrosis as indicated by decrease in trypan blue-positive myocytes and leakage of lactate dehydrogenase compared with untreated cells after either SI or SI-RO. The number of terminal deoxynucleotidyl transferase-mediated nick end labeling-positive myocytes or loss of JC-1 fluorescence following SI and 18 h of RO was attenuated in the sildenafil-treated group with concomitant inhibition of caspase 3 activity. An early increase in Bcl-2 to Bax ratio with sildenafil treatment was also observed in myocytes after SI-RO. The increase of Bcl-2 expression by sildenafil was inhibited by nitric-oxide synthase (NOS) inhibitor, L-nitro-amino-methyl-ester. The drug also enhanced mRNA and protein content of inducible NOS (iNOS) and endothelial NOS (eNOS) in the myocytes. Sildenafil-induced protection against necrosis and apoptosis was absent in the myocytes derived from iNOS knock-out mice and was attenuated in eNOS knock-out myocytes. The up-regulation of Bcl-2 expression by sildenafil was also absent in iNOS-deficient myocytes. Reverse transcription-PCR, Western blots, and immunohistochemical assay confirmed the expression of phosphodiesterase-5 in mouse cardiomyocytes. These data provide strong evidence for a direct protective effect of sildenafil against necrosis and apoptosis through NO signaling pathway. The results may have possible therapeutic potential in preventing myocyte cell death following ischemia/reperfusion.

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Section: Resultsmentioning

confidence: 99%

Phosphodiesterase-5 Inhibitor Sildenafil Preconditions Adult Cardiac Myocytes against Necrosis and Apoptosis

Das

Xi²,

Kukreja

2005

Journal of Biological Chemistry

320

276

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“…Also in animal models of heart failure, both the inhibition of I NHE by cariporide and of late I Na by ranolazine reduced [Na + ] i and improved EC coupling and LV remodeling [6,34,38,62,163,202]. In conditions of cardiac ischemia/reperfusion, inhibition of I NHE preserved mitochondrial energetics (i.e., ATP and PCr content) [111,162]. However, these effects were not related to an improvement of EC coupling, but rather to a delay of mitochondrial matrix acidification by a mechanism unrelated to the sarcolemmal NHE [162].…”

Section: Discussionmentioning

confidence: 99%

“…In conditions of cardiac ischemia/reperfusion, inhibition of I NHE preserved mitochondrial energetics (i.e., ATP and PCr content) [111,162]. However, these effects were not related to an improvement of EC coupling, but rather to a delay of mitochondrial matrix acidification by a mechanism unrelated to the sarcolemmal NHE [162]. Furthermore, beneficial effects of ranolazine on mitochondrial energetics have so far been related to its ability to decrease fatty-acid oxidation, promote glucose oxidation, and by increasing pyruvate dehydrogenase complex activity [1,125,192] rather than by improving EC coupling.…”

Section: Discussionmentioning

confidence: 99%

Excitation-contraction coupling and mitochondrial energetics

Maack

O’Rourke²

2007

Basic Res Cardiol

218

183

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Cardiac excitation-contraction (EC) coupling consumes vast amounts of cellular energy, most of which is produced in mitochondria by oxidative phosphorylation. In order to adapt the constantly varying workload of the heart to energy supply, tight coupling mechanisms are essential to maintain cellular pools of ATP, phosphocreatine and NADH. To our current knowledge, the most important regulators of oxidative phosphorylation are ADP, P i , and Ca 2+ . However, the kinetics of mitochondrial Ca 2+ -uptake during EC coupling are currently a matter of intense debate. Recent experimental findings suggest the existence of a mitochondrial Ca 2+ microdomain in cardiac myocytes, justified by the close proximity of mitochondria to the sites of cellular Ca 2+ release, i. e., the ryanodine receptors of the sarcoplasmic reticulum. Such a Ca 2+ microdomain could explain seemingly controversial results on mitochondrial Ca 2+ uptake kinetics in isolated mitochondria versus whole cardiac myocytes. Another important consideration is that rapid mitochondrial Ca 2+ uptake facilitated by microdomains may shape cytosolic Ca 2+ signals in cardiac myocytes and have an impact on energy supply and demand matching. Defects in EC coupling in chronic heart failure may adversely affect mitochondrial Ca 2+ uptake and energetics, initiating a vicious cycle of contractile dysfunction and energy depletion. Future therapeutic approaches in the treatment of heart failure could be aimed at interrupting this vicious cycle. Keywords calcium; sodium; microdomain; heart failure; adenosine triphosphate; adenosine diphosphate; respiration; tricarboxylic acid cycle Physiological aspectsThe most important function of the heart is to pump blood to supply the body with oxygen and substrates. In order to adapt cardiac output to the constantly changing demand of blood supply, the heart utilizes three major mechanisms to increase cardiac output: the force-frequency relationship (the Bowditch effect or Treppe; [22]), the Frank-Starling mechanism (sarcomere length-dependent activation of contractile force) [66,149,164], and sympathetic activation [28]. All of these mechanisms increase and accelerate myocardial force generation, and at the same time increase cellular energy demand. By these mechanisms, cardiac output during exertion can be increased more than five-fold compared to resting conditions. © Steinkopff Verlag 2007Correspondence to: Christoph Maack. NIH Public Access Excitation-contraction couplingOf fundamental importance for cardiac contraction and relaxation are the processes of excitation-contraction (EC) coupling (Fig. 1). During the action potential (AP), voltage-gated Na + -channels are activated, and the inward Na + -current (I Na ) induces a rapid depolarization of the cell membrane, facilitating voltage-dependent opening of L-type Ca 2+ -channels (I Ca,L ). The Ca 2+ influx triggers the opening of the ryanodine receptor (RyR2 subtype), inducing the release of even greater amounts of Ca 2+ from the sarcoplasmic reticulum (SR), a process te...

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“…Changes in mitochondrial pH were monitored after abrupt removal of Na + from an "intracellular-like" medium containing the following: 135mM KCl, 10mM NaCl, 0.5mM KH 2 PO 4 , 0.5mM MgCl 2 , and 20mM HEPES (pH 7.2), as well as 10 μM digitonin 22 . The experiments were performed in the presence or absence of 20 μM HMA and 20 μM EIPA, two NHE inhibitors 23 , to evaluate the possible involvement of NHA-oc/NHA2.…”

Section: Intramitachondrial (H + ) Measurementsmentioning

confidence: 99%

“…Mitochondrial NHEs have been reported to mediate Na + acetate-induced increases in matrix volume, also referred to as "passive swelling" 22 . To test whether NHA-oc/NHA2 has a similar activity, RAW 264 cells were stimulated with RANKL and transfected with a mixture of two nha-oc/NHA2-specific siRNA molecules.…”

Section: Nha-oc/nha2 Mediates Matrix Swelling In Isolated Mitochondriamentioning

confidence: 99%

NHA-oc/NHA2: A mitochondrial cation–proton antiporter selectively expressed in osteoclasts

Battaglino¹,

Pham²,

Morse

et al. 2008

Bone

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Bone resorption is regulated by a complex system of hormones and cytokines that cause osteoblasts/stromal cells and lymphocytes to produce factors including RANKL, that ultimately result in the differentiation and activation of osteoclasts, the bone resorbing cells.We used a microarray approach to identify genes upregulated in RANKL-stimulated osteoclastprecursor cells. Osteoclast expression was confirmed by multiple tissue Northern and in situ hybridization analysis. Gene function studies were carried out by siRNA analysis.We identified a novel gene, which we termed nha-oc/NHA2, which is strongly upregulated during RANKL-induced osteoclast differentiation in vitro and in vivo. nha-oc/NHA2 encodes a novel cation/proton antiporter (CPA), and is the mouse orthologue of a human gene identified in a database search: HsNHA2. nha-oc/NHA2 is selectively expressed in osteoclasts. NHA-oc/NHA2 protein localizes to the mitochondria, where it mediates Na + -dependent changes in mitochondrial pH and Na + Acetate induced-mitochondrial passive swelling. RNA silencing of nha-oc/nha2 reduces osteoclast differentiation and resorption, suggesting a role for NHA-oc/NHA2 in these processes.nha-oc/NHA2 therefore is a novel member of the CPA family, and is the first mitochondrial NHA characterized to date. nha-oc/NHA2 is also unique in that it is the first eukaryotic and tissue specific CPA2 characterized to date. NHA-oc/NHA2 displays the expected activities of a bona fide CPA and plays a key role(s) in normal osteoclast differentiation and function.

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Cariporide preserves mitochondrial proton gradient and delays ATP depletion in cardiomyocytes during ischemic conditions

Cited by 88 publications

References 32 publications

Phosphodiesterase-5 Inhibitor Sildenafil Preconditions Adult Cardiac Myocytes against Necrosis and Apoptosis

Phosphodiesterase-5 Inhibitor Sildenafil Preconditions Adult Cardiac Myocytes against Necrosis and Apoptosis

Excitation-contraction coupling and mitochondrial energetics

NHA-oc/NHA2: A mitochondrial cation–proton antiporter selectively expressed in osteoclasts

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