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Albumin
therapy of transient focal cerebral ischemia: in vivo analysis of dynamic
microvascular responses.
Belayev L, Pinard E, Nallet H,
Seylaz J, Liu Y, Riyamongkol P, Zhao W, Busto R, Ginsberg
MD.
Stroke 2002 Apr;33(4):1077-84
Cerebral
Vascular Disease Research Center, Department of Neurology, University of Miami
School of Medicine, Miami, Fla 33101, USA.
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BACKGROUND AND PURPOSE: To study whether
intravascular or hemodynamic factors contribute to the marked neuroprotective
effect of albumin therapy in focal cerebral ischemia, 2 complementary methods
were applied: laser-scanning confocal microscopy (LSCM) and laser-Doppler
perfusion imaging (LDPI). METHODS: In the LSCM study, Sprague-Dawley rats were
anesthetized with halothane/nitrous oxide, and a cranial window was placed over
the dorsolateral frontoparietal cortex. Rats received 2-hour middle cerebral
artery occlusion (MCAO) by an intraluminal suture and were treated with human
albumin (1.25 g/kg; n=4) or saline (n=3) after 30 minutes of recirculation.
Video images of cortical vessels were continually acquired and were digitized
offline to measure diameters and fluorescent erythrocyte velocities. In the LDPI
study, cortical perfusion was measured in anesthetized Sprague-Dawley rats that
received 2-hour MCAO and were treated with albumin (2.5 g/kg; n=6) or saline
(n=5) at 30 minutes after recirculation. RESULTS: In the LSCM study, MCAO was
associated with arteriolar dilation and slowing of capillary and venular
erythrocyte perfusion. During the first 15 to 30 minutes of postischemic
recirculation, prominent foci of vascular stagnation developed within cortical
venules, associated with thrombuslike foci and adherent corpuscular structures
consistent in size with neutrophils. Saline administration failed to affect
these phenomena, while albumin therapy was followed by significant increases in
arteriolar diameter ( approximately 12%; P=0.007) and by a prompt improvement of
venular and capillary erythrocyte perfusion and a partial disappearance of
adherent thrombotic material. Albumin therapy increased erythrocyte flow
velocity in both capillaries (288+/-73% versus 76+/-18% in the saline group;
P=0.023) and venules (2.7-fold [P=0.001] versus 1.0-fold in the saline group
[P=NS]). In the LDPI study, cortical perfusion declined during MCAO and rose
initially with recirculation (to approximately 135% of baseline) in both groups.
Mean cortical perfusion improved slightly (approximately 14%; P=NS) in
albumin-treated animals. CONCLUSIONS: These results reveal a beneficial effect
of albumin therapy in reversing stagnation, thrombosis, and corpuscular
adherence within cortical venules in the reperfusion phase after focal ischemia
and support its utility in the treatment of acute ischemic stroke.
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