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European Journal of Cardio-Thoracic Surgery, Vol 2, 244-255, Copyright © 1988 by European Association for Cardio-thoracic Surgery
W Flameng, W Dyszkiewicz and J Minten
Long-term preservation of dog hearts was performed over 24 h using
Bretschneider-HTK cardioplegia and cold storage. Preservation was assessed
in terms of conservation of myocardial tissue levels of high- energy
phosphates (HEP) and functional outcome after cardiac transplantation.
Serial left ventricular biopsies were taken and analysed for ATP, ADP, AMP,
adenosine, inosine, hypoxanthine, xanthine and creatine phosphate.
Myocardial structure was studied by electron microscopical examination of a
similar biopsy specimen. Cardiac performance was measured before and after
cardiac transplantation. Several techniques of cardioplegic arrest were
studied: single dose cardioplegia, multidose cardioplegia and continuous
perfusion with the cardioplegic solution. In all groups, the hearts were
stored at 0.5 degree C for 24 h. In the group of single dose
Bretschneider-HTK cardioplegia, myocardial ATP content after 24 h of cold
storage was only 25% of control. The total sum of nucleotides at that time
interval was however 65% of the control value. Reperfusion of these hearts
using a support dog (whole blood reperfusion) did not result in any
recovery of ATP. Creatinine phosphate however showed an overshoot.
Accumulated nucleosides were washed out. The hearts showed electrical
activity but were severely arrhythmic. Contractility was poor. In the group
of multidose Bretschneider-HTK cardioplegia, HEP preservation was better
than after single dose cardioplegia. ATP content was about 50% of control.
The total sum of nucleotides was 85% of control. Ultrastructural assessment
of the myocytes revealed only slight ischaemic damage to the mitochondria.
Reperfusion on cardiopulmonary bypass after cardiac transplantation did not
show any restoration of ATP, but a steady catabolism of HEP. The
nucleosides adenosine and inosine were not washed out upon reperfusion.
After cardiac transplantation, none of these hearts could be weaned from
cardiopulmonary bypass due to irreversible low cardiac output. Histological
examination demonstrated irreversible myocardial tissue damage. In the
group of continuous cold Bretschneider cardioplegia, HEP content was
completely preserved throughout the 24 h of perfusion. Ultrastructure of
the myocytes was normal. Reperfusion of the transplanted hearts showed a
mild breakdown of ATP to 70% of control values accompanied by a slight
accumulation of nucleosides. Haemodynamic recovery however was perfect and
none of the hearts needed positive inotropic support. Myocytes after
reperfusion had a normal subcellular appearance.(ABSTRACT TRUNCATED AT 400
WORDS)
ARTICLES
Energy state of the myocardium during long-term cold storage and subsequent reperfusion
K. U. Leuven, Laboratory of Experimental Cardiac Surgery, Belgium.
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