Influence of the ph of cardioplegic solutions on cellular energy metabolism and hydrogen ion flux during neonatal hypothermic circulatory arrest and reperfusion: A dynamic 31p nuclear magnetic resonance study in a pig model

Objectives: The pH of cardioplegic solutions is postulated to affect myocardial protection during neonatal hypothermic circulatory arrest. Neither optimization of cardioplegic pH nor its influence on intracellular pH during hypothermic circulatory arrest has been previously studied in vivo. Thus we...

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Veröffentlicht in:The Journal of thoracic and cardiovascular surgery 1997-10, Vol.114 (4), p.601-608
Hauptverfasser: Portman, Michael A., Panos, Anthony L., Xiao, Yun, Anderson, David L., Alfieris, George M., Ning, Xue-Han, Lupinetti, Flavian M.
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Sprache:eng
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Zusammenfassung:Objectives: The pH of cardioplegic solutions is postulated to affect myocardial protection during neonatal hypothermic circulatory arrest. Neither optimization of cardioplegic pH nor its influence on intracellular pH during hypothermic circulatory arrest has been previously studied in vivo. Thus we examined the effects of the pH of cardioplegic solutions on postischemic cardiac function in vivo, including two possible operative mechanisms: (1) reduction in adenosine triphosphate use and depletion of high-energy phosphate stores or (2) reduction of H + flux during reperfusion, or both. Methods: Dynamic 31P spectroscopy was used to measure rates of adenosine triphosphate use, high-energy phosphate depletion, cytosolic acidification during hypothermic circulatory arrest, and phosphocreatine repletion and realkalinization during reperfusion. Neonatal pigs in three groups ( n = 8 each)—group A, acidic cardioplegia (pH = 6.8); group B, basic cardioplegia (pH = 7.8); and group N, no cardioplegia—underwent hypothermia at 20° C with 60 minutes of hypothermic cardioplegia followed by reperfusion. Results: Recoveries of peak elastance, stroke work, and diastolic stiffness were superior in group B. Indices of ischemic adenosine triphosphate use, initial phosphocreatine depletion rate, and τ, the exponential decay half-time, were not different among groups. Peak [H +] in group A (end-ischemia) was significantly elevated over that of group B. The realkalinization rate was reduced in group B compared with that in groups A ( p = 0.015) and N ( p = 0.035), with no difference between groups A and N ( p = 0.3). Cytosolic realkalinization rate was markedly reduced and the half-time of [H +] decay was increased during reperfusion in group B. Conclusions: Superior postischemic cardiac function in group B is not related to alterations in ischemic adenosine triphosphate use or high-energy store depletion, but may be due to slowing in H + efflux during reperfusion, which should reduce Ca ++ and Na + influx. (J Thorac Cardiovasc Surg 1997;114:601-8)
ISSN:0022-5223
1097-685X
DOI:10.1016/S0022-5223(97)70050-3