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| This article is part of the supplement: 18th Spring Meeting of the Association of Cardiothoracic AnaesthetistsMeeting abstractSuppression of interleukin-8 and myeloperoxidase production in the cerebrovascular bed during repeated deep hypothermic circulatory arrest1Papworth Hospital, Cambridge, UK 2University of Cambridge, UK Cambridge, UK. 22 June 2001 Critical Care 2001, 5(Suppl C):1doi:10.1186/cc1030
© 2001 BioMed Central Ltd IntroductionIt has been suggested that mild hypothermia during cardiopulmonary bypass (CPB) may attenuate, but not completely suppress, the production of interleukin-8 (IL-8) in the brain [1]. This study examined the effect of repeated deep hypothermic circulatory arrest (DHCA) on production of IL-8 and myeloperoxidase (MPO) in the cerebrovascular bed in patients undergoing pulmonary thromboendarterectomy (PTE). MethodsAfter LREC approval and written informed consent, we studied eight patients undergoing PTE. Anaesthetic and surgical technique were strictly standardized [2] and all patients had a jugular bulb catheter inserted after induction. After initiation of CPB, all patients were cooled to below 20°C and underwent at least two periods of DHCA for 20 min. Each DHCA period was separated by a 10-min reperfusion interval. The levels of IL-8 and MPO were measured in paired arterial and jugular samples drawn simultaneously at specific time points, using enzyme-linked immunoassay kits. Juguloarterial (j-a) gradients were then calculated. All data are expressed as median (interquartile range) and were compared with the baseline values using the Wilcoxon signed rank sum test. J-a gradients were compared with zero using one-sample t-test. ResultsThe baseline arterial values before CPB [T1] for IL-8 and MPO were 12.9 (11.5-21.4)pg/ml and 4.5 (3.1-6.6)ng/ml, respectively (Fig. 1). For both IL-8 and MPO, arterial levels significantly increased before the first DHCA [T3] to 28.3 (21.6-43.1)pg/ml and 31.2 (26.1-11.7)ng/ml, respectively, and remained elevated until 8 min following the second DHCA [T7]. However, no significant j-a differences for IL-8 and MPO were found throughout this period.
ConclusionsThese data imply that the cerebral activation of inflammatory processes represented as specific IL-8 and MPO production in the cerebrovascular bed are suppressed during repeated DHCA in the present study. References
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Figure 1.