Circulation, Vol 72, 1177-1184, Copyright © 1985 by American Heart Association
C Patrono, G Ciabattoni, P Patrignani, F Pugliese, P Filabozzi, F Catella, G Davi and L Forni
Nonsteroidal anti-inflammatory drugs and sulfinpyrazone compete dose-
dependently with arachidonate for binding to platelet cyclooxygenase. Such
a process closely follows systemic plasma drug concentrations and is
reversible as a function of drug elimination. Peak inhibition and extent of
its reversibility at 24 hr varies consistently with individual
pharmacokinetic profile. Inhibition of platelet cyclooxygenase activity by
these agents is associated with variable effects on prostaglandin (PG)
synthesis in the gastric mucosa and the kidney. Aspirin acetylates platelet
cyclooxygenase and permanently inhibits thromboxane (TX) A2 production in a
dose-dependent fashion when single doses of 0.1 to 2.0 mg/kg are given.
Acetylation of the enzyme by low-dose aspirin is cumulative on repeated
dosing. The fractional dose of aspirin necessary to achieve a given level
of acetylation by virtue of cumulative effects approximately equals the
fractional daily platelet turnover. Serum TXB2 measurements obtained during
long-term dosing with 0.11, 0.22, and 0.44 mg/kg aspirin in four healthy
subjects could be fitted by a theoretical model assuming identical
acetylation of platelet (irreversible) and megakaryocyte (reversible)
cyclooxygenase. For a given dose within this range, both the rate at which
cumulative acetylation occurs and its maximal extent largely depend upon
the rate of platelet turnover. Continuous administration of low-dose
aspirin (20 to 40 mg/day) has no statistically significant effect on
urinary excretion of either 6-keto- PGF1 alpha or 2,3-dinor-6-keto-PGF1
alpha, i.e., indexes of renal and extrarenal PGI2 biosynthesis in vivo.
Whether a selective sparing of extraplatelet cyclooxygenase activity by
low-dose aspirin will result in increased antithrombotic efficacy, fewer
toxic reactions, or both remains to be established in prospective clinical
trials.
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