HCO3−-Dependent Intracellular pH Regulation in the Premature Myocardium

This study investigated developmental changes in Na+-H+ exchange and HCO3 -Cl exchange activities in newborn and adult rabbit hearts. pHi was measured using the fluorescent dye 2ʼ,7ʼ-bis(2-carboxyethyl)-5(6)-carboxyfluorescein in isolated myocytes. Myocardial mechanical function was measured in the isolated ventricular preparation. Intracellular acidosis with normal pH. was induced by an NH4Cl (10 mM) prepulse technique. Upon removal of NH4Cl, pHi fell transiently and then recovered toward the control level. In the HCO3-/CO2-buffered solution, the rate of recovery of pH; in the newborn was greater than in the adult. In the HCO3-/CO2-buffered solution, 5-(N-ethyl-N-isopropyl)amiloride (EIPA), an inhibitor of Na+-H+ exchange, inhibited the recovery of pHi completely in the adult. In the newborn, however, significant recovery of pHi was observed in the presence of EIPA. In the presence of both EIPA and 4-acetamido-4ʼ-isothiocyanatostilbene-2ʼ,2ʼ-disulfonic acid (SITS), an inhibitor of HCO3-Cl exchange, the recovery of pHi was not observed in the two age groups. In the HEPES-buffered solution that did not contain HCO3-/CO2, the rate of recovery of pHi after NH4Cl removal was similar in the two age groups. In the HEPES-buffered solution, the recovery of pHi was completely inhibited by EIPA in the two age groups. In the presence of EIPA in the HCO3/CO2-buffered solution, contractile function decreased during acidosis after NH4Cl removal and did not recover in the adult. In the newborn, significant recovery of contractile function was observed after NH4Cl removal in the presence of EIPA. The recovery of mechanical function observed in the presence of EIPA in the newborn was inhibited by SITS. These data suggest that, although there is no developmental change in the Na+-H+ exchange activity, HCO3-Cl exchange is more active in the premature myocardium. The presence of the HCO3-Cl- exchanger is important in maintaining myocardial contractile function during acidosis, especially when Na+-H+ exchange is inhibited and may partly explain the greater resistance of the premature myocardium to acidosis.