Clinical efficacy of buprenorphine after oral dosing in rats undergoing major surgery

Author:

Nordén Einar Sjaastad12,Veras Ioanni3,Yadav Prakash4,Løken Kari4,Dishington Hilde12,Thorstensen Christian5,Sjaastad Ivar12,Rasmussen Henrik46ORCID

Affiliation:

1. Institute for Experimental Medical Research, Oslo University Hospital, Norway

2. K. G. Jebsen Centre for Cardiac Research, University of Oslo, Norway

3. Department of Molecular Medicine, University of Oslo, Norway

4. Department of Comparative Medicine, Oslo University Hospital, Norway

5. Department of Pharmacology, Oslo University Hospital, Norway

6. Institute of Clinical Medicine, University of Oslo, Norway

Abstract

Serum corticosterone, serum buprenorphine, body weight change, consumption of food and water and behaviour-based pain assessment were measured in catheterised and non-catheterised male Wistar rats undergoing myocardial infarct (MI) surgery under general anaesthesia following buprenorphine dosing by subcutaneous (Bup-SC, 0.05 mg/kg) and oral (Bup-O, 0.4 mg/kg) routes. Buprenorphine was dosed subcutaneously at half an hour before and 8, 16 and 24 hours after surgery (Bup-SC), orally at one hour before surgery (Bup-O1) or at one hour before and 12 hours after surgery (Bup-O2) in catheterised rats and at one hour before and 24 hours after surgery (Bup-O24) in non-catheterised rats. Serum corticosterone, body weight changes and food and water consumption were not significantly different between treatments in catheterised rats. Bup-SC resulted in rapidly decreasing serum concentrations below the clinically effective concentrations (1 ng/mL) already at two hours after the first dose. Bup-O provided significantly higher and slowly decreasing serum concentrations, at or above clinically effective concentrations, for 24 hours (Bup-O1) and 42 hours (Bup-O2) after surgery. In non-catheterised rats, body weight development and food consumption were significantly higher in Bup-O24 rats compared to Bup-SC rats. The results indicate that a SC buprenorphine dose of 0.05 mg/kg every eight hours provides long periods of serum concentrations below clinically effective levels, and that a higher dose and/or more frequent dosage are required to provide stable serum concentrations at or above clinically effective levels. A single oral buprenorphine dose of 0.4 mg/kg provides clinically effective and stable serum concentrations for 24 hours in rats after MI surgery.

Funder

This study was supported by research funds from Oslo University Hospital.

Publisher

SAGE Publications

Subject

General Veterinary,Animal Science and Zoology

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