Cancers (Jun 2021)

Population Pharmacokinetics of Oxycodone and Metabolites in Patients with Cancer-Related Pain

  • Bram C. Agema,
  • Astrid W. Oosten,
  • Sebastiaan D.T. Sassen,
  • Wim J.R. Rietdijk,
  • Carin C.D. van der Rijt,
  • Birgit C.P. Koch,
  • Ron H.J. Mathijssen,
  • Stijn L.W. Koolen

DOI
https://doi.org/10.3390/cancers13112768
Journal volume & issue
Vol. 13, no. 11
p. 2768

Abstract

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Oxycodone is frequently used for treating cancer-related pain, while not much is known about the factors that influence treatment outcomes in these patients. We aim to unravel these factors by developing a population-pharmacokinetic model to assess the pharmacokinetics of oxycodone and its metabolites in cancer patients, and to associate this with pain scores, and adverse events. Hospitalized patients with cancer-related pain, who were treated with oral oxycodone, could participate. Pharmacokinetic samples and patient-reported pain scores and occurrence and severity of nine adverse events were taken every 12 h. In 28 patients, 302 pharmacokinetic samples were collected. A one-compartment model for oxycodone and each metabolite best described oxycodone, nor-oxycodone, and nor-oxymorphone pharmacokinetics. Furthermore, oxycodone exposure was not associated with average and maximal pain scores, and oxycodone, nor-oxycodone, and nor-oxymorphone exposure were not associated with adverse events (all p > 0.05). This is the first model to describe the pharmacokinetics of oxycodone including the metabolites nor-oxycodone and nor-oxymorphone in hospitalized patients with cancer pain. Additional research, including more patients and a more timely collection of pharmacodynamic data, is needed to further elucidate oxycodone (metabolite) pharmacokinetic/pharmacodynamic relationships. This model is an important starting point for further studies to optimize oxycodone dosing regiments in patients with cancer-related pain.

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