Hypertension, Vol 5, 307-311, Copyright © 1983 by American Heart Association
T Odori, A Paskins-Hurlburt and NK Hollenberg
Studies to assess the role of blood pressure rise in the growth of the
collateral arterial supply following renal artery stenosis were performed
in 70 rats. Assessment of the proliferative response was made by coded
reading of endothelial cell turnover following tritiated thymidine
administration, 5 days after renal artery stenosis. Stenosis induced the
anticipated brisk increase in endothelial cell turnover in arterial
collaterals and in the ipsilateral renal vein, and ureteric epithelium.
Blood pressure elevation did not appear to play the dominant role, as the
proliferative response did not parallel blood pressure changes; moreover,
neither bilateral renal artery stenosis, designed to enhance the
hypertension, nor hydralazine administration, to reduce the blood pressure,
influenced endothelial cell turnover. A contribution of elevated blood
pressure to the vasoproliferative response, however, was not ruled out
definitively in this study. Captopril, also administered to assess the same
question, resulted in an enhanced endothelial cell proliferative response,
both in frequency and in degree, an observation that became the central
thrust of our study. The mechanism by which converting enzyme inhibitor
modified endothelial cell turnover is not clear, but may well provide
insight into the responsible factors.
ARTICLES
Increase in collateral arterial endothelial cell proliferation induced by captopril after renal artery stenosis in the rat