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The International Brain Hypothermia Symposium 2004was the second
time I have had the honor of opening such a gathering on brain
hypothermia treatment. It was a great pleasure to greet the
participants in the hope that their valuablecontributions would
make the Tokyo meeting memorable. Brainhypothermia has long been
seen as a promising method that may overcome current limitations on
brain resuscitation in patients with severe brain damage. However,
although excellentresults have been obtained in experimental animal
models, for some reason brain hypothermia has not alwaysbeen
successful clinically, and resolving this problem has been a major
challenge facing physicians specializing in brain therapies. The
ICUmanagement of recent research has uncovered newmechanisms
ofbrain damage not seen in animal models, including brain
thermo-pooling at temperatures above 40 C in severe brain damage,
masking neuronal hypoxia even with normal cerebral blood flow.
Stress-related hyper glycemia with brain hypothermia was expected
to generate useful results in patients with external injuries,
cerebral occlusive stroke, and cardiac arrest. In recent clinical
studies of brain hypothermia treatment, many excellent results
began being reported on the manage ment of severe brain injury,
ischemic stroke, and post-resuscitation after cardiac arrest.
However, in clinical brain hypothermia treatment many questions
remained about appro priate treatment targets, leu management
technique, prevention of complications, control of brain tissue
temperature, management of hypothermia insult, and mechanisms
underly ing the onset of vegetative states."
The International Brain Hypothermia Symposium 2004was the second
time I have had the honor of opening such a gathering on brain
hypothermia treatment. It was a great pleasure to greet the
participants in the hope that their valuablecontributions would
make the Tokyo meeting memorable. Brainhypothermia has long been
seen as a promising method that may overcome current limitations on
brain resuscitation in patients with severe brain damage. However,
although excellentresults have been obtained in experimental animal
models, for some reason brain hypothermia has not alwaysbeen
successful clinically, and resolving this problem has been a major
challenge facing physicians specializing in brain therapies. The
ICUmanagement of recent research has uncovered newmechanisms
ofbrain damage not seen in animal models, including brain
thermo-pooling at temperatures above 40 C in severe brain damage,
masking neuronal hypoxia even with normal cerebral blood flow.
Stress-related hyper glycemia with brain hypothermia was expected
to generate useful results in patients with external injuries,
cerebral occlusive stroke, and cardiac arrest. In recent clinical
studies of brain hypothermia treatment, many excellent results
began being reported on the manage ment of severe brain injury,
ischemic stroke, and post-resuscitation after cardiac arrest.
However, in clinical brain hypothermia treatment many questions
remained about appro priate treatment targets, leu management
technique, prevention of complications, control of brain tissue
temperature, management of hypothermia insult, and mechanisms
underly ing the onset of vegetative states."
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