Switching from high doses of pure µ-opioid agonists to transdermal buprenorphine in patients with cancer: A feasibility study

Authors

  • Lena Lundorff, MD
  • Per Sjøgren, DmSci, MD
  • Ole Bo Hansen, MD
  • Torsten Jonsson, MD
  • Per Rotbøll Nielsen
  • Lona Christrup, PhD, MSc(Pharm)

DOI:

https://doi.org/10.5055/jom.2013.0166

Keywords:

cancer patients, transdermal buprenorphine, opioid switching

Abstract

Background: Several myths on buprenorphine’s pharmacology exist: possible analgesic ceiling effect, feasibility of combination with other opioid agonists, and the reversibility of side effects. Aim to evaluate: 1) if cancer patients receiving high doses of pure agonists could obtain adequate pain relief after switching to transdermal (TD) buprenorphine and 2) whether the numbers of breakthrough pain episodes after switching increased and whether they could be treated with the same doses of pure agonist as before switching.

Design: The prospective open multicenter study included outpatients with moderate-to-severe cancer pain satisfactorily controlled.

Setting: Patients were switched from the usual pure agonist to TD buprenorphine and were titrated to a stable dose. The assessments were: 1) daily self-assessment of pain intensity, numbers of rescue medications, and pain interference with sleep; 2) brief pain inventory; 3) pain relief and pain intensity; 4) quality of life; and 5) adverse events and symptoms.

Results: Eighteen patients receiving 150-516 mg of morphine/day were included. The buprenorphine dose at the end of the study varied between 52.5 and 140 mg/h. No difference in pain before and after switching was shown. The level of rescue doses was maintained. The patches were well tolerated. A significant decrease in fatigue and an increase in global health status were seen after the switch.

Conclusion: It is feasible to switch cancer patients from high doses of pure µ- opioid agonists to TD buprenorphine without eliciting any antagonist effects, but the dose conversion factor is individual and the switching process should be tailored for the individual patient.

Author Biographies

Lena Lundorff, MD

Consultant, Department of Palliative Care, Herning, Denmark; Department of Palliative Care, Uddevalla, Sweden

Per Sjøgren, DmSci, MD

Professor, Consultant, Section of Palliative Medicine, Rigshospitalet, Copenhagen, Denmark

Ole Bo Hansen, MD

Consultant, Palliative and Pain Clinic, Holbæk Sygehus, Denmark.

Torsten Jonsson, MD

Consultant, Multidisciplinary Pain Centre, Køge Hospital, University of Copenhagen, Copenhagen, Denmark.

Per Rotbøll Nielsen

Multidisciplinary Pain Centre, Rigshospitalet, Denmark

Lona Christrup, PhD, MSc(Pharm)

Professor, Department of Drug Design and Pharmacology, University of Copenhagen, Copenhagen, Denmark.

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Published

07/01/2013

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Section

Articles