Circulation, Vol 83, 1380-1389, Copyright © 1991 by American Heart Association
H Hanke, KK Haase, S Hanke, M Oberhoff, S Hassenstein, E Betz and KR Karsch
BACKGROUND. Little is known about the mechanism(s) in the development of
restenosis after excimer laser angioplasty. Thus, the rationale of this
study was to determine the time course of intimal and medial smooth muscle
cell (SMC) proliferation and histomorphological changes after experimental
excimer laser treatment. METHODS AND RESULTS. Laser ablation was performed
in the right carotid artery of 34 New Zealand White rabbits after
development of a fibromuscular plaque by repeated weak electrical
stimulations. The vessels were excised 3, 7, 14, 21, 28, and 42 days after
excimer laser treatment. Staining of alpha-actin was used to identify SMCs.
In five rabbits (15%), a stenosis of more than 50% of luminal area was due
to intimal proliferation of SMCs, and in four other rabbits, a total
occlusion was due to organized thrombi. After the initial ablation of the
performed plaque (13 +/- 6 intimal SMC layers) a continuous increase of
intimal wall thickness was found from 7 +/- 6 SMC layers at 7 days to 28
+/- 5 intimal SMC layers at 28 days after excimer laser ablation (p less
than 0.01). After 42 days, no additional increase of intimal thickening
occurred. After bromodeoxyuridine labeling, the extent of cell
proliferation (percent of cells undergoing DNA synthesis) in the intima and
media was determined using a monoclonal antibody against bromodeoxyuridine.
Immunohistological quantification of SMC proliferation in the intima
revealed a significant increase of cells undergoing DNA synthesis at 3 (p
less than 0.05) and 14 (p less than 0.01) days after laser treatment.
Medial proliferation of SMCs was delayed and had a significant increase 7
days (p less than 0.05) after intervention. Twenty-one days after laser
treatment, SMC proliferation in the intima as well as in the media was
normalized. CONCLUSIONS. The proliferative response of SMCs after
experimental excimer laser treatment will occur as a dynamic process with a
maximum of SMCs undergoing DNA synthesis during 14 days after laser
ablation, resulting in an increase of intimal thickening within 4 weeks
after laser treatment. The extent of intimal hyperplasia due to SMC
proliferation after excimer laser treatment is comparable with the effect
of transluminal balloon angioplasty in this experimental model.
ARTICLES
Morphological changes and smooth muscle cell proliferation after experimental excimer laser treatment
Department of Medicine, University of Tubingen, FRG.
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