Stroke, Vol 14, 219-226, Copyright © 1983 by American Heart Association
A Ames 3d and FB Nesbett
Rabbit retina was used as an example of organized central nervous tissue in
in vitro experiments designed to characterize the onset of cell death from
ischemia. Retinas were subjected to progressively longer periods of
different types of ischemic insult and then given an opportunity to recover
before being tested for irreversible damage, using failure to reinstitute
protein synthesis as the principal criterion. Anoxia was more damaging than
substrate deprivation, but they were synergistic in combination.
Restricting the volume of extracellular fluid during the combined
deprivation, to simulate complete circulatory arrest in vivo, caused
irreversible damage to occur even sooner. The cells were able to recover
from 20 min of the complete ischemia, but it took them more than 2 h to do
so. After 30 min, there was extensive irreversible damage. Loss of
viability was usually associated with failure to reinstitute energy
metabolism, as assessed by 2-deoxyglucose uptake. Under some circumstances
loss of viability may have been the consequence of the failed energy
metabolism. Increasing medium Mg++, prior to ischemia, to levels that
greatly reduce energy requirements caused a significant improvement in the
recovery of 2-deoxyglucose uptake.
ARTICLES
Pathophysiology of ischemic cell death: I. Time of onset of irreversible damage; importance of the different components of the ischemic insult
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