Hypertension, Vol 4, 590-596, Copyright © 1982 by American Heart Association
FA Mendelsohn, J Csicsmann, JS Hutchinson, R DiNicolantonio and Y Takata
Angiotensin-converting enzyme (ACE) in rat brain closely resembled that in
lung in its kinetics with the substrate Hip-His Leu, the inhibitors SQ
20,881 and SQ 14,225, and iun its Cl- activation profile. Modification of
dietary NaCl intake was associated with marked changes in brain ACE
activity. Sodium-loaded rats had lower activity of ACE in hypothalamus,
striatum, and midbrain, and higher activity in spinal cord compared to
controls. In sodium-restricted rats, ACE was elevated in pituitary and
depressed in spinal cord. Chronic intravenous infusion of angiotensin (AII)
was associated with a pattern of changes partly resembling sodium loading:
ACE was depressed in hypothalamus and striatum but elevated in midbrain.
After chronic intracerebroventricular infusion of AII, ACE was elevated in
striatum and hippocampus, and depressed in spinal cord; a pattern of
changes quite different from those associated with intravenous AII. These
results show that ACE in several brain regions is sensitive to dietary
sodium intake and support the hypothesis that angiotensin-containing
neurons in these areas might be responsive to NaCl status of the animal.
The observed changes in brain ACE do not seem to be explained in any simple
manner by changes in circulating or central angiotensin II.
ARTICLES
Modulation of brain angiotensin-converting enzyme by dietary sodium and chronic intravenous and intracerebroventricular fusion of angiotensin II