Effects of AM281, a cannabinoid antagonist, on systemic haemodynamics, internal carotid artery blood flow and mortality in septic shock in rats

doi:10.1093/bja/aei106

BJA Advance Access published online on February 25, 2005
British Journal of Anaesthesia, doi:10.1093/bja/aei106

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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: journal.permissions@oupjournals.org
Accepted January 10, 2005

Laboratory Investigation

Effects of AM281, a cannabinoid antagonist, on systemic haemodynamics, internal carotid artery blood flow and mortality in septic shock in rats

Y. Kadoi ¹^*, H. Hinohara ¹, F. Kunimoto ¹, H. Kuwano ¹, S. Saito ², and F. Goto ²

¹ Department of Intensive Care, Gunma University, Graduate School of Medicine, 3-39-22 Showa-machi, Maebashi, Gunma 371-8511, Japan
² Department of Anesthesiology, Gunma University, Graduate School of Medicine, 3-39-22 Showa-machi, Maebashi, Gunma 371-8511, Japan

^* To whom correspondence should be addressed.
Y. Kadoi, E-mail: kadoi{at}med.gunma-u.ac.jp

Abstract

Introduction. The purpose of this study was to examine the effectsof AM281, a cannabinoid receptor antagonist, on systemic haemodynamics,internal carotid artery blood flow and mortality during septicshock in rats.

Methods. The study included three sets of experiments:measurements of changes in systemic haemodynamics and left internalcarotid artery flow (30 animals divided into three groups of10); measurements of biochemical variables (n=30); assessmentof mortality (n=30). Male Wistar rats (7 weeks old) were randomlydivided into three groups: group 1, control; group 2, lipopolysaccharide(LPS) i.v., Escherichia coli endotoxin 10.0 mg kg^-1 i.v., bolus;group 3, LPS 10.0 mg kg^-1 i.v.+AM281 1 mg kg^-1 i.v. Systemichaemodynamics, carotid artery flow changes and biochemical variableswere assessed at pretreatment and 1, 2 and 3 h after the treatmentwas performed.

Results. Administration of AM281 could preventthe haemodynamic changes induced by sepsis. Tumour necrosisfactor- ${alpha}$ and interleukin 1- ${beta}$ increased in the LPS i.v. and LPSi.v.+AM281 groups at 1, 2 and 3 h after treatment; significantdifferences were observed in these levels in the two groupsat these times. Internal carotid artery blood flow remainedfairly constant in the control and LPS i.v.+AM281 groups comparedwith baseline values. In the LPS i.v. group, it decreased at2 and 3 h after the treatment compared with baseline values[at 2 h: control 12.7 (SD 0.9) ml min^-1, LPS i.v. 8.7 (1.4)ml min^-1 (P<0.05), LPS i.v.+AM281 11.5 (0.9) ml min^-1; at3 h: control 12.7 (0.4) ml min^-1, LPS i.v. 7.7 (1.3) ml min^-1(P<0.05), LPS i.v.+AM281 11.6 (1.0) ml min^-1]. Significantdifferences in mortality within 6 and 12 h were found betweenthe LPS i.v. and LPS i.v.+AM281 groups [6 h mortality: LPS i.v.5/10 (50%), LPS i.v.+AM281 2/10 (20%), P<0.05; 12 h mortality:LPS i.v. group 10/10 (100%), LPS i.v.+AM281 5/10 (50%), P<0.05].

Conclusions.Administration of AM281 prevented changes in systemic haemodynamicand internal carotid artery blood flow and could improve mortalityin experimentally induced septic shock in rats. These findingsmay have significant therapeutic implications in the treatmentof septic shock.

Keywords: carotid artery, blood flow; complications, sepsis; model, rat; pharmacology, cannabinoids.

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