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The Journal of Thoracic and Cardiovascular Surgery, Vol 96, 717-724, Copyright © 1988 by The American Association for Thoracic Surgery and The Western Thoracic Surgical Association
JE Baker, LE Boerboom and GN Olinger
Hypothermia combined with pharmacologic cardioplegia protects the globally
ischemic adult heart, but this benefit may not extend to children; poor
postischemic recovery of function and increased mortality may result when
this method of myocardial protection is used in children. The relative
susceptibilities to ischemia-induced injury modified by hypothermia alone
and by hypothermia plus cardioplegia were assessed in isolated perfused
immature (7- to 10-day-old) and mature (6- to 24-month-old) rabbit hearts.
Hearts were perfused aerobically with Krebs-Henseleit buffer in the working
mode for 30 minutes, and aortic flow was recorded. This was followed by 3
minutes of hypothermic (14 degrees C) coronary perfusion with either Krebs
or St. Thomas' Hospital cardioplegic solution No. 2, followed by
hypothermic (14 degrees C) global ischemia (mature hearts 2 and 4 hours;
immature hearts 2, 4, and 6 hours). Hearts were reperfused for 15 minutes
in the Langendorff mode and 30 minutes in the working mode, and recovery of
postischemic function was measured. Hypothermia alone provided excellent
protection of the ischemic immature rabbit heart, with recovery of aortic
flow after 2 and 4 hours of ischemia at 97% +/- 3% and 93% +/- 4% (mean +/-
standard deviation) of the preischemic value. Mature hearts protected with
hypothermia alone recovered only minimally, with 22% +/- 16% recovery of
preischemic aortic flow after 2 hours; none were able to generate flow at 4
hours. St. Thomas' Hospital solution No. 2 improved postischemic recovery
of aortic flow after 2 hours of ischemia in mature hearts from 22% +/- 16%
to 65% +/- 6% (p less than 0.05), but actually decreased postischemic
aortic flow in immature hearts from 97% +/- 3% to 86% +/- 10% (p less than
0.05). To investigate any dose- dependency of this effect, we subjected
hearts from both age groups to reperfusion with either Krebs solution or
St. Thomas' Hospital solution No. 2 for 3 minutes every 30 minutes
throughout a 2-hour period of ischemia. Reexposure to Krebs solution during
ischemia did not affect postischemic function in either age group.
Reexposure of immature hearts to St. Thomas' Hospital solution No. 2 caused
a decremental loss of postischemic function in contrast to incremental
protection with multidose cardioplegia in the mature heart. We conclude
that immature rabbit hearts are significantly more tolerant of ischemic
injury than mature rabbit hearts and that, unexpectedly, St. Thomas'
Hospital solution No. 2 damages immature rabbit hearts.
ARTICLES
Age-related changes in the ability of hypothermia and cardioplegia to protect ischemic rabbit myocardium
Department of Cardiothoracic Surgery, Medical College of Wisconsin, Milwaukee.
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