AJP - Cell Physiology, Vol 259, Issue 1 C169-C179, Copyright © 1990 by American Physiological Society
Acidification and intracellular sodium ion activity during stimulated myocardial ischemia
B. Vanheel, A. de Hemptinne and I. Leusen
Laboratory of Normal and Pathological Physiology, University of Gent, Belgium.
With the use of microelectrodes, intracellular pH (pHi), surface pH (pHs),
and intracellular Na+ activity (aiNa) were measured in isolated guinea pig
papillary muscles during normal superfusion and during a reversible
condition of simulated ischemia. Acid loading by NH+4 prepulse or by
CO2-HCO3- addition during superfusion with pH 7.4 solutions caused internal
acidification followed by a recovery of pHi, which could be inhibited by
amiloride. pHi recovery was associated with an amiloride-sensitive peak
rise of aiNa and membrane hyperpolarization, indicative of Na(+)-H+
exchange. Peak increase of aiNa was absent if the pH of the superfusion
solution was concomitantly lowered. Imposed ischemia after control
superfusion caused membrane depolarization and acidification of pHi and
pHs. The change of pHs consistently was larger than that of pHi. aiNa
decreased from 5.5 to 4.6 mM after 10-min ischemia. Enlarging the pHi (and
pHs) decrease in ischemia by prior reduction of the tissue buffer capacity
(CO2-HCO3(-)-free superfusion) was unable to induce a rise of aiNa during
the subsequent ischemic period. Amiloride had no significant effect on aiNa
during ischemia. It is concluded that the important acidification of pHs
reduces the rate of pHi regulatory Na(+)-H+ exchange and thereby
contributes to a longer maintenance of the Na+ electrochemical gradient in
ischemic cardiac muscle.
