Hypertension, Vol 7, 491-498, Copyright © 1985 by American Heart Association
N Kohashi, NC Trippodo, AA MacPhee, ED Frohlich and FE Cole
The inhibitory effect of high and low molecular weight native and synthetic
rat atrial peptides on oxygen consumption in isolated rat kidney
mitochondria and slices was measured. Oxygen consumption by mitochondria
was measured in the presence of succinate and/or adenosine diphosphate,
furosemide, and low and high molecular weight native and synthetic rat
atrial peptides. After the addition of succinate, adenosine diphosphate
limiting respiration (State 4) increased in the presence of low, but not
high, molecular weight native rat atrial peptides. Furosemide caused a
significant decrease in State 4 respiration (p less than 0.001).
Angiotensin II and arginine vasopressin did not alter State 4 respiration.
The rate of oxygen consumption after the addition of saturating adenosine
diphosphate in the presence of saturating succinate (State 3 respiration)
was reduced by low and high molecular weight native rat atrial peptides.
Furosemide completely blocked oxygen consumption after the addition of
adenosine diphosphate. Oxygen consumption was unchanged by trypsin treated
(natriuretically inactive) low molecular weight rat atrial peptides and
ventricular protein extracts of high and low molecular weight native rat
atrial peptides. Synthetic and low molecular weight native rat atrial
peptides had similar effects on mitochondrial oxygen consumption. Low
molecular weight native and synthetic rat atrial peptides decreased the
adenosine diphosphate to oxygen ratio, and these peptides, as well as
furosemide, also induced mitochondrial swelling; none of the other rat
atrial peptide combinations nor angiotensin II produced this effect. In
kidney slices, basal oxygen consumption (without substrates) was stimulated
by succinate.(ABSTRACT TRUNCATED AT 250 WORDS)
ARTICLES
Rat atrial natriuretic peptides inhibit oxygen consumption by rat kidney