Impaired autoregulation in an experimental model of chronic cerebral hypoperfusion in rats

Impaired autoregulation in an experimental model of chronic cerebral hypoperfusion in rats

To verify the hypothesis that impaired autoregulation may contribute to cerebral swelling or hemorrhage after a sudden recovery of perfusion pressure, we studied the chronic effects of cerebral hypoperfusion on the autoregulatory responses of the pial arterioles in situ. Eight to 12 weeks after a ca...

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Published in:Stroke (1970) Vol. 27; no. 8; pp. 1399 - 1404
Main Authors: Irikura, K, Morii, S, Miyasaka, Y, Yamada, M, Tokiwa, K, Yada, K
Format: Journal Article
Language:English
Published: United States American Heart Association, Inc 01-08-1996
Subjects:
Animals
Arteriovenous Fistula - surgery
Brain Ischemia - physiopathology
Carotid Arteries - physiopathology
Cerebrovascular Circulation - physiology
Chronic Disease
Disease Models, Animal
Homeostasis - physiology
Hypercapnia - physiopathology
Hypertension - physiopathology
Hypocapnia - physiopathology
Jugular Veins - physiopathology
Male
Microcirculation - physiology
Pia Mater - blood supply
Pia Mater - physiopathology
Pressure
Rats
Rats, Sprague-Dawley
Regional Blood Flow
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Summary:To verify the hypothesis that impaired autoregulation may contribute to cerebral swelling or hemorrhage after a sudden recovery of perfusion pressure, we studied the chronic effects of cerebral hypoperfusion on the autoregulatory responses of the pial arterioles in situ. Eight to 12 weeks after a carotid-jugular fistula was created in rats, experiments were performed under alpha-chloralose and urethane anesthesia. Regional cerebral blood flow (rCBF) was determined by the hydrogen clearance method, and carotid pressure was measured. Using a closed cranial window, we determined the autoregulatory responses of the arterioles (30 to 50 microns) to both hypertension induced by norepinephrine and sudden fistula closure at various mean arterial pressures (MAPs). rCBF on the fistula side was reduced by 27%. Carotid pressure was significantly lower than normal but was immediately increased by fistula closure. The pial arterioles showed marked elongation and enlargement. During induced hypertension, the arterioles in the fistula group started to dilate at an MAP lower than that of the control group (130 versus 180 mm Hg, respectively). The arterioles constricted when the fistula was occluded at normal MAP. However, when the fistula was occluded at an MAP higher than 130 mm Hg, the vessels dilated. It was demonstrated that (1) chronic hypoperfusion induced impairment of the upper limit of autoregulation and (2) sudden fistula closure under hypertensive conditions caused vasodilation of the arterioles. These findings suggest that rapid restoration of perfusion pressure is possibly followed by a pressure breakthrough phenomenon in a chronically hypoperfused cerebrovasculature.
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ISSN:0039-2499
1524-4628
DOI:10.1161/01.str.27.8.1399