Effects of mitochondrial KATP modulators on cardioprotection induced by chronic high altitude hypoxia in rats

doi:10.1016/S0008-6363(02)00456-X

Cardiovascular Research 2002 55(3):567-575; doi:10.1016/S0008-6363(02)00456-X
© 2002 by European Society of Cardiology

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Effects of mitochondrial K_ATP modulators on cardioprotection induced by chronic high altitude hypoxia in rats

Jan Necká $r$ ^a, Ondrej Szárszoi^a, Luká $s$ Koten^a, Franti $s$ ek Papou $s$ ek^a, Bohuslav O $s$ t'ádal^a, Gary J Grover^b and Franti $s$ ek Kolá $r$ ^a^,*

^aInstitute of Physiology, Academy of Sciences of the Czech Republic and Centre for Experimental Cardiovascular Research, Víde $n$ ská 1083, 142 20 Prague 4, Czech Republic
^bMetabolic and Cardiovascular Diseases Drug Discovery, Bristol-Myers Squibb Pharmaceutical Research Institute, Pennington, NJ, USA

^* Corresponding author. Tel.: +420-2-4106-2559; fax: +420-2-4106-2125 kolar{at}biomed.cas.cz

Objectives: Adaptation of rats to intermittent high altitudehypoxia increases the tolerance of their hearts to acute ischemia/reperfusioninjury. Our aim was to examine the role of mitochondrial ATP-sensitivepotassium channels (K_ATP) in this form of protection. Methods:Adult male Wistar rats were exposed to hypoxia of 5000 m ina barochamber for 8 h/day, 5 days a week; the total number ofexposures was 24–32. A control group was kept under normoxicconditions (200 m). Infarct size (tetrazolium staining) wasmeasured in anesthetized open-chest animals subjected to 20-minregional ischemia (coronary artery occlusion) and 4-h reperfusion.Isolated perfused hearts were used to assess the recovery ofcontractile function following 20-min global ischemia and 40-minreperfusion. In the open-chest study, a selective mitochondrialK_ATP blocker, 5-hydroxydecanoate (5 mg/kg), or openers, diazoxide(10 mg/kg) or BMS-191095 (10 mg/kg), were administered intothe jugular vein 5 and 10 min before occlusion, respectively.In the isolated heart study, 5-hydroxydecanoate (250 µmol/l)or diazoxide (50 µmol/l) were added to the perfusion medium5 or 10 min before ischemia, respectively. Results: In the controlnormoxic group, infarct size occupied 62.2±2.0% of thearea at risk as compared with 52.7±2.5% in the chronicallyhypoxic group (P<0.05). Post-ischemic recovery of contractilefunction (dP/dt) reached 60.0±3.9% of the pre-ischemicvalue and it was improved to 72.4±1.2% by adaptationto hypoxia (P<0.05). While 5-hydroxydecanoate completelyabolished these protective effects of chronic hypoxia, it hadno appreciable influence in normoxic groups. In contrast, diazoxidesignificantly increased the recovery of contractile functionand reduced infarct size in normoxic groups only. The latereffect was also observed following treatment with BMS-191095.Conclusion: The results suggest that opening of mitochondrialK_ATP channels is involved in the cardioprotective mechanismconferred by long-term adaptation to intermittent high altitudehypoxia.

KEYWORDS Contractile function; Hypoxia/anoxia; Infarction; Ischemia; K-ATP channel; Mitochondria; Reperfusion

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