Hypertension, Vol 16, 655-661, Copyright © 1990 by American Heart Association
J Geoffroy, D Benzoni, M Vincent and J Sassard
To determine whether the increased renal biosynthesis of thromboxane A2
observed in young genetically hypertensive rats of the Lyon strain could be
involved in the development of their hypertension, Lyon hypertensive female
rats received either thromboxane synthetase inhibitors (Dazmegrel or OKY
046) or a thromboxane A2 receptor antagonist (AH 23848) during their
prehypertensive stage. Treatment from 5 to 9 weeks of age with Dazmegrel
failed to reduce systolic blood pressure. When given from 3 to 9 weeks of
age, Dazmegrel and OKY 046 induced a similar progressive and specific
reduction (60%) in the urinary excretion of thromboxane B2 that was
associated with a transient decrease in blood pressure level with Dazmegrel
and a longer lasting blood pressure-lowering effect with OKY 046. AH 23848,
given according to the same schedule, normalized the blood pressure level.
This effect persisted 1 week after the cessation of the treatment.
Interestingly, active doses of thromboxane synthetase inhibitors or of
thromboxane A2 receptor blocker required a 3-week delay to exhibit their
antihypertensive properties. It is concluded that 1) the elevated
production of thromboxane A2 observed in young Lyon hypertensive rats is
likely to participate actively in their blood pressure regulation and 2)
this effect may be independent of its direct vasoconstrictor properties.
ARTICLES
Thromboxane A2 and development of genetic hypertension in the Lyon rat strain
Department of Physiology and Clinical Pharmacology, Faculty of Pharmacy, Lyon, France.
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