Effects of prophylactic or therapeutic application of bovine haemoglobin HBOC-200 on ischaemia-reperfusion injury following acute coronary ligature in rats{dagger}

doi:10.1093/bja/aei255

BJA Advance Access published online on October 14, 2005
British Journal of Anaesthesia, doi:10.1093/bja/aei255

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© The Board of Management and Trustees of the British Journal of Anaesthesia 2005. All rights reserved. For Permissions, please e-mail: journals.permissions@oxfordjournals.org
Accepted August 30, 2005

Laboratory Investigation

Effects of prophylactic or therapeutic application of bovine haemoglobin HBOC-200 on ischaemia-reperfusion injury following acute coronary ligature in rats

M. A. Burmeister ¹^* , C. Rempf ¹, T. G. Standl ¹ , S. Rehberg ¹, S. Bartsch-Zwemke ¹, T. Krause ¹, S. Tuszynski ¹, A. Gottschalk ¹, and J. Schulte am Esch ¹

¹ Department of Anaesthesia, University Medical Center Hamburg-Eppendorf, Martinistrasse 52, D-20246 Hamburg, Germany

^* To whom correspondence should be addressed.
M. A. Burmeister, E-mail: burmeister{at}uke.uni-hamburg.de

Abstract

Background. Haemoglobin-based oxygen carriers (HBOCs) are assessedas blood substitutes in patients with perioperative anaemiaincluding patients at risk for perioperative cardiac ischaemia.There is controversy as to whether HBOCs are beneficial or deleteriousduring ischaemia-reperfusion (I-R). Therefore the effects ofHBOC-200 on I-R injury were evaluated in a randomized placebo-controlledanimal trial.

Methods. Animals were randomized to receive eitherplacebo i.v. without I-R (sham group, n=9), placebo i.v. withI-R (control group, n=10), HBOC-200 0.4 g kg^-1 i.v. prior toI-R (prophylaxis group, n=12) or HBOC-200 0.4 g kg^-1 i.v. duringI-R (therapy group, n=15). I-R consisted of 25 min of acuteligature of the left coronary artery followed by 120 min ofreperfusion. Measurements included assessment of the area atrisk and infarct size using triphenyl tetrazolium chloride (TTC)stain, DNA single-strand breaks (in situ nick translation withautoradiography/densitometry) and cardiac arrhythmias.

Results.Infarct size within the area at risk was 62 (SD 15)% (control),46 (10)% (prophylaxis, P<0.025 vs control) and 61 (9)% (therapy,P<0.85 vs control). The frequency of DNA single-strand breakswas reduced vs control in the sham (P<0.01) and prophylaxis(P<0.04) groups and was almost the same in the therapy group(P<0.75). The severity of cardiac arrhythmias during ischaemiawas lower compared with control in the sham (P<0.001) andprophylaxis (P<0.039) groups, but there was no differencein the therapy group.

Conclusion. This study demonstrates thatneither prophylactic nor therapeutic application of the cell-freehaemoglobin solution HBOC-200 aggravates cardiac I-R injury.Furthermore, the prophylactic approach may offer a new opportunityfor pretreatment of patients at risk for perioperative ischaemiccardiac events.

Keywords: blood, haemoglobin; heart, arrhythmia; heart, ischaemia; model, rat; special drugs.

The results were presented in part at the Congress of the European Society of Anaesthesia, Glasgow, UK, June 2003 (‘Best Abstract Award’), and at the Annual Meeting of the American Society of Anesthesiologists, San Francisco, CA, USA, October 2003.

Declaration of interest. T. G. Standl has received lecture honoraria and travel fees from Biopure Corporation, Boston, MA, the manufacturer of HBOC. The Department of Anaesthesiology, University Hospital, Hamburg-Eppendorf, received restricted grants from Biopure Corporation, Boston, MA, between 1994 and 1998 for animal and clinical phase II and III trials. M.A. Burmeister is Vice President Research and Development, Hospital Care Division, B. Braun Melsungen AG, Melsungen, Germany. B. Braun, a global health care supplier, cooperated with Biopure Corporation, Boston, MA, on HBOC development until 1996. The work presented in this paper was done independently of and without any support from B. Braun.

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