Journal of Applied Physiology, Vol 62, Issue 4 1582-1588, Copyright © 1987 by American Physiological Society
Effects of acetazolamide on cerebrospinal fluid ions in metabolic alkalosis in dogs
S. Javaheri
We hypothesized that inhibition of carbonic anhydrase in the central
nervous system by acetazolamide should limit the rise in cisternal
cerebrospinal fluid (CSF) [HCO3-] observed in metabolic alkalosis. To test
this hypothesis, isosmotic isonatremic metabolic alkalosis was produced in
two groups of anesthetized, paralyzed, and mechanically ventilated dogs (8
in each group). Group II animals received 50 mg/kg of acetazolamide
intravenously 1 h before induction of metabolic alkalosis of 5-h duration.
Renal effects of acetazolamide were eliminated by ligation of renal
pedicles. In both groups cisternal CSF [Na+] remained relatively constant
during metabolic alkalosis. In group I CSF [Cl-] decreased 3.6 and 8.2
meq/l, respectively, 2.5 and 5 h after induction of metabolic alkalosis.
Respective increments in CSF [HCO3-] were 3.4 and 6.0 meq/l. In
acetazolamide-treated dogs, during metabolic alkalosis, increments in CSF
[HCO3-] (4.8 and 7.2 meq/l, respectively, at 2.5 and 5 h) and decrements in
CSF [Cl-] (9.1 and 13.3 meq/l) were greater than those observed in group I.
We conclude that, in dogs with metabolic alkalosis and bilateral ligation
of renal pedicles, acetazolamide impairs CSF regulation of HCO3- and Cl-
ions; acetazolamide not only failed to impede HCO3- rise but actually
appeared to increase it. The mechanisms for these observations are
discussed.
