Circulation, Vol 69, 1161-1170, Copyright © 1984 by American Heart Association
LR Bush, WB Campbell, LM Buja, GD Tilton and JT Willerson
Recent studies suggest that platelet activation and subsequent thromboxane
(TX) A2 release play important roles in certain coronary syndromes. To
further test this possibility, we examined the ability of a selective
TXA2-synthetase inhibitor, dazoxiben (UK-37-248), to abolish cyclic flow
reductions (CFRs) that occur in experimentally stenosed canine coronary
arteries. CFRs, which are characterized by progressive declines in coronary
blood flow and interrupted by sudden and usually spontaneous restorations
of flow, were produced by placing hard plastic cylindrical constrictors (5
mm long X 4.5 mm outer diameter) on the proximal left anterior descending
or circumflex coronary artery in open-chest, anesthetized dogs. Coronary
blood flow was measured with pulsed Doppler flow probes placed proximal to
the constrictors and regional myocardial blood flow with 15 micron
radiolabeled microspheres. CFRs were observed for 1 hr, during which
coronary blood flow was monitored continuously. Regional myocardial blood
flow was measured before constriction, when coronary blood flow appeared to
be at its nadir, and after spontaneous restorations of flow. After 1 hr
dazoxiben (2.5 mg/kg iv) or an equal volume of saline was given and
coronary blood flow was monitored for another hour. Dazoxiben abolished
CFRs completely in 18 of 28 dogs and significantly reduced their frequency
in the dogs receiving the drug (10.1 +/- 0.8 vs 3.2 +/- 1.0 per hour [+/-
SE]; p less than .001, n = 28). The frequency and magnitude of variations
in cyclic blood flow were unchanged after saline (8.8 +/- 0.8 vs 9.0 +/-
1.0 per hour; p = NS, n = 13). The lowest levels of coronary blood flow
before and after dazoxiben were 8.6 +/- 2.2% and 48.8 +/- 5.4% of control,
respectively (p less than .001, n = 28), whereas this parameter remained
unchanged after saline (18.7 +/- 5.7% vs 13.4 +/- 4.1%, respectively; n =
13). The levels of TXB2 and 6-keto-prostaglandin (PG) F1 alpha (stable
breakdown products of TXA2 and prostacyclin, respectively) were measured in
blood collected from aortic and distal coronary arterial catheters before
coronary constriction (control), during CFRs, and after administration of
dazoxiben. TXB2 levels measured distal to the stenosis were increased
fivefold during CFRs (352 +/- 126 vs 71 +/- 18 pg/ml plasma; p less than
.03) and were reduced to preconstriction (control) levels by dazoxiben (57
+/- 12 pg/ml). Aortic TXB2 levels almost doubled with CFRs and also
returned to control levels after dazoxiben.(ABSTRACT TRUNCATED AT 400
WORDS)
ARTICLES
Effects of the selective thromboxane synthetase inhibitor dazoxiben on variations in cyclic blood flow in stenosed canine coronary arteries
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