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European Journal of Cardio-Thoracic Surgery, Vol 10, 774-783, Copyright © 1996 by European Association for Cardio-thoracic Surgery
W Martin, R Carter, A Tweddel, J Belch, M el-Fiky, AM McQuiston, M McLaren and DJ Wheatley
OBJECTIVE: Cardiopulmonary bypass induces respiratory dysfunction
postoperatively, with activation of both the complement system and white
cells implicated. This study compared the effects of bubble and membrane
oxygenators for cardiopulmonary bypass in terms of respiratory dysfunction
and markers of white cell activation and endothelial damage. METHODS: Fifty
patients undergoing cardiopulmonary bypass were randomly allocated either
membrane or bubble oxygenation. Respiratory function was assessed serially
by arterial oxygen tension and alveolar- arterial oxygen gradient.
Complement activation was measured by serial sampling of serum C3a levels.
White cell activation was assessed by serial measurement granulocyte
elastase; other markers investigated were levels of thromboxane B2, von
Willebrand factor and malondialdehyde. All sample measurements were made
preoperatively, early and late during bypass, 4-6 h postoperatively and
then on the 1st, 2nd and 6th postoperative day. All samples were corrected
for haemodilution, and differences between groups tested non-
parametrically. RESULTS: In both groups of patients there was a highly
significant fall (P < 0.001) in arterial oxygen tension accompanied by a
highly significant rise (P < 0.0001) in aleveolar-arterial oxygen
gradient at 18 h compared to preoperative values persisting until 6 days
postoperatively. Levels of C3a increased significantly in both groups at 10
min post bypass, increased further at 60 min peaking at 4- 6 h post bypass.
Granulocyte elastase serum levels increased significantly at 10 min
postoperatively in both groups compared to control levels, remaining
elevated till 48 h, but returning to control levels by 6 days. There was a
small difference (P < 0.04) between the groups at 4-6 h only. Levels of
von Willebrand factor increased significantly at 60 min post bypass in both
groups, remaining elevated 6 days postoperatively. Levels of
malondialdehyde increased at 10 min post bypass, remaining elevated until 6
days post bypass. Thromboxane levels showed no significant changes. For all
markers measured, there were no significant differences between the groups
other than those already indicated. CONCLUSIONS: This study demonstrated
marked respiratory dysfunction, complement activation and white cell
activation in patients undergoing cardiopulmonary bypass with either bubble
or membrane oxygenators. There was marked variability in the response of
individual patients with either oxygenation technique, but overall no
significant differences between the groups.
ARTICLES
Respiratory dysfunction and white cell activation following cardiopulmonary bypass: comparison of membrane and bubble oxygenators
Department of Cardiac Surgery, Glasgow Royal Infirmary, University NHS Trust, Scotland.
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