Prevention of ischemic rigor contracture during coronary occlusion by inhibition of Na+–H+ exchange

Garcı́a-Dorado, David; Ma, González; Barrabés, José A.; Ruiz‐Meana, Marisol; Solares, Julia; Rm, Lidón; Blanco, José Manuel Soto; Puigfel, Yolanda; Piper, H. M.; Soler‐Soler, Jordi

doi:10.1016/s0008-6363(97)00106-5

Cited by 90 publications

(57 citation statements)

References 27 publications

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“…The protective effect of cariporide against cell death secondary to ischemiareperfusion was, therefore, fully explained in this model by its effect on ATP decay during the ischemic period. This result is consistent with previous studies showing that cariporide needs to be present during the ischemic period to be protective (6,16).…”

Section: Discussionsupporting

confidence: 93%

“…Slowed ATP depletion during ischemic conditions. The present observations in cultured cardiomyocytes exposed to simulated ischemia and in intact myocardium submitted to zero-flow ischemia are in agreement with previous studies showing that NHE inhibition slows-down the rate of ATP depletion during ischemia and delays the onset of rigor contracture (6,11,25). Moreover, in the present study, modulation of the rate of ATP depletion during ischemia by modifying myocardial temperature within the physiological range (35.5-38.5°C) allowed us to evaluate the contribution of the effect of cariporide on ATP content to its protective effect against ischemia-reperfusion injury.…”

Section: Discussionsupporting

confidence: 93%

“…In a recent study (31), pretreatment with the selective NHE inhibitor SM-20550 was associated with attenuated Ca 2ϩ overload in mitochondria obtained from rat hearts submitted to 40 min of ischemia and 20 min of reperfusion, a result in agreement with the protective effect of NHE inhibition against cell necrosis secondary to ischemia-reperfusion, but [Ca 2ϩ ] m during ischemia was not measured. Our observation that cariporide, at concentrations that have been consistently found cardioprotective in isolated cells (25,27) and intact myocardium in vivo (6,16), enhanced mitochondrial Ca 2ϩ accumulation during simulated ischemia may appear surprising. Although increased [Ca 2ϩ ] m has been shown to have detrimental effects (4), there is a lack of information on the consequences of mitochondrial Ca 2ϩ overload during ischemia.…”

Section: Discussionmentioning

confidence: 86%

“…However, the observed delay in pH recovery is very small, and other studies (27) have shown that the NaHCO 3 cotransporter may compensate for NHE inhibition, allowing a rapid normalization of intracellular pH during reperfusion. Although with some discrepancies (10), studies in different models have shown that to be effective, NHE inhibition must act during coronary occlusion (6,16) or cardioplegia (28), whereas its application at the time of reperfusion affords little, if any, protection against cell death. Recent reports (6,18,25) indicate that NHE inhibition delays the progression of ischemic injury as manifested by ATP depletion or development of rigor contracture.…”

Section: /Hmentioning

confidence: 99%

“…Although with some discrepancies (10), studies in different models have shown that to be effective, NHE inhibition must act during coronary occlusion (6,16) or cardioplegia (28), whereas its application at the time of reperfusion affords little, if any, protection against cell death. Recent reports (6,18,25) indicate that NHE inhibition delays the progression of ischemic injury as manifested by ATP depletion or development of rigor contracture. It has been suggested that NHE1 is markedly inhibited during severe ischemia (23).…”

Section: /Hmentioning

confidence: 99%

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

Ruiz‐Meana

Garcı́a-Dorado

Pina

et al. 2003

American Journal of Physiology-Heart and Circulatory Physiology

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The mechanism by which inhibition of Na ϩ /H ϩ exchanger (NHE) reduces cell death in ischemic-reperfused myocardium remains controversial. This study investigated whether cariporide could inhibit mitochondrial NHE during ischemia, delaying H ϩ gradient dissipation and ATP exhaustion. Mouse cardiac myocytes (HL-1) were submitted to 1 h of simulated ischemia (SI) with NaCN/deoxyglucose (pH 6.4), with or without 7 M cariporide, and mitochondrial concentration of Ca 2ϩ (Rhod-2), 2Ј,7Ј-bis(2-carboxyethyl)-5(6)-carboxyfluorescein (BCECF) and the charge difference across the mitochondrial membrane potential (⌬⌿m, JC-1) were assessed. ATP content was measured by bioluminescence and mitochondrial swelling by spectrophotometry in isolated mitochondria. Cariporide significantly attenuated the acidification of the mitochondrial matrix induced by SI without modifying ⌬⌿m decay, and this effect was associated to a delayed ATP exhaustion and increased mitochondrial Ca 2ϩ load. These effects were reproduced in sarcolemma-permeabilized cells exposed to SI. In these cells, cariporide markedly attenuated the fall in mitochondrial pH induced by removal of Na ϩ from the medium. In isolated mitochondria, cariporide significantly reduced the rate and magnitude of passive matrix swelling induced by Na ϩ acetate. In isolated rat hearts submitted to 40-min ischemia at different temperatures (35.5°, 37°, or 38.5°C) pretreatment with cariporide limited ATP depletion during the first 10 min of ischemia and cell death (lactate dehydrogenase release) during reperfusion. These effects were mimicked when a similar ATP preservation was achieved by hypothermia and were abolished when the sparing effect of cariporide on ATP was suppressed by hyperthermia. We conclude that cariporide acts at the mitochondrial level, delaying mitochondrial matrix acidification and delaying ATP exhaustion during ischemia. These effects can contribute to reduce cell death secondary to ischemia-reperfusion.

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Section: Discussionsupporting

confidence: 93%

Section: Discussionsupporting

confidence: 93%

Section: Discussionmentioning

confidence: 86%

Section: /Hmentioning

confidence: 99%

Section: /Hmentioning

confidence: 99%

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

Ruiz‐Meana

Garcı́a-Dorado

Pina

et al. 2003

American Journal of Physiology-Heart and Circulatory Physiology

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Electrical Plasticity and Cardioprotection in Myocardial Ischemia—Role of Selective Sodium Channel Blockers

Madonna¹,

Çevik²,

Nasser³

2013

Clinical Cardiology

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The concept of electrical protection of the ischemic myocardium is in constant evolution and has recently been supported by experimental and clinical studies. Historically, antiplatelet agents, angiotensin‐converting enzyme inhibitors, β‐blockers, and statins have been all proposed as drugs conferring anti‐ischemic cardioprotection. This was supported by the evidence consistently indicating that all these drugs were capable of reducing mortality and the risk of repeat myocardial infarction. The electrical plasticity paradigm is, however, a novel concept that depicts the benefits of improved sodium channel blockade with drugs such as ranolazine and cariporide. Although it has been hypothesized that the protective role of ranolazine depends on decreased fatty acid β‐oxidation affecting preconditioning, we speculate against such a hypothesis, because inhibition of β‐oxidation requires higher concentrations of the drug, above the therapeutic range. Rather, we discuss the key role of calcium overload reduction through inhibition of the late sodium current (INa). Mechanisms driving cardioprotection involve the block of a cascade of complex ionic exchanges that can result in intracellular acidosis, excess cytosolic calcium, myocardial cellular dysfunction, and eventually cell injury and death. In this review we discuss the studies that demonstrate how electrical plasticity through sodium channel blockers can promote cardioprotection against ischemia in coronary heart disease.

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Blocking Na+–H+Exchange by Cariporide Reduces Na+-overload in Ischemia and is Cardioprotective

Hartmann¹,

Decking²

1999

Journal of Molecular and Cellular Cardiology

108

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Prevention of ischemic rigor contracture during coronary occlusion by inhibition of Na+–H+ exchange

Cited by 90 publications

References 27 publications

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

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

Electrical Plasticity and Cardioprotection in Myocardial Ischemia—Role of Selective Sodium Channel Blockers

Blocking Na+–H+Exchange by Cariporide Reduces Na+-overload in Ischemia and is Cardioprotective

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