Improved Opioid Analgesic Effect Following Opioid Dose Reduction
Version of Record online: 20 AUG 2008
© American Academy of Pain Medicine
Volume 9, Issue 6, pages 724–727, September 2008
How to Cite
Vorobeychik, Y., Chen, L., Bush, M. C. and Mao, J. (2008), Improved Opioid Analgesic Effect Following Opioid Dose Reduction. Pain Medicine, 9: 724–727. doi: 10.1111/j.1526-4637.2008.00501.x
- Issue online: 20 AUG 2008
- Version of Record online: 20 AUG 2008
Vol. 9, Issue 8, 1228, Version of Record online: 19 NOV 2008
- Opioid-Induced Hyperalgesia;
- Cancer Pain;
- Chronic Pain;
- NMDA Receptor Antagonist
Introduction. Traditionally, opioids have been the cornerstone of therapy for patients suffering from cancer pain, regardless of the potential to develop opioid tolerance. In chronic pain patients who experience worsening pain despite increasing doses of opioids, the clinical role of opioid-induced hyperalgesia is gaining more recognition.
Case. Presented here is the case of a 56-year-old man with recurrent squamous cell lung carcinoma and spinal metastases, suffering with intractable 8/10 pain on the visual analog scale in his chest, lower thoracic spine, and upper lumbar spine. He was admitted five times for pain control. In spite of escalating doses of oxycodone, morphine, and hydromorphone, the patient continued to experience severe pain. Also, he endured undesirable sedation, fatigue, and generalized weakness. The clinical picture suggested the possibility of opioid-induced hyperalgesia. We decreased the hydromorphone dose by 40–50% and started methadone. The patient's pain level dropped to a more acceptable 3/10. He was more alert, and his pain was tolerable until his death.
Discussion. Opioid-induced hyperalgesia might be considered in a patient who has no evidence of disease progression, who is on clinically reasonable doses of opioids, and whose pain escalates as opioid doses are increased. A reduction of opioids and the addition of a low-dose N-methyl-D-aspartate receptor antagonist may provide a favorable clinical outcome in those patients who have failed to benefit from opioid rotation and other adjunctive pain treatments.