Long-term safety, tolerability, and efficacy of OROS® hydromorphone in patients with chronic pain
DOI:
https://doi.org/10.5055/jom.2009.0011Keywords:
chronic pain, long-term management, hydromorphone, safety, tolerability, efficacyAbstract
Objective: To assess the safety and efficacy of long-term repeated dosing of OROS® hydromorphone in chronic pain patients.Design: This multicenter, open-label extension trial enrolled patients from three short-term OROS® hydromorphone trials.
Setting: Fifty-six centers in the United States and Canada.
Patients: Adults with chronic cancer pain or chronic nonmalignant pain who were receiving stable doses of OROS® hydromorphone (≥8 mg/day). Three hundred and eighty-eight patients were enrolled, 106 patients completed at least 12 months of therapy.
Interventions: OROS® hydromorphone (individualized doses) was administered once daily.
Main outcome measures: Safety and efficacy (Brief Pain Inventory and patient and investigator global evaluations) were assessed at monthly visits.
Results: The median duration of extended OROS® hydromorphone therapy was 274 days. The median daily dose of study medication was 32.0 mg at extension-study baseline, 40.0 mg at month 3, and 48.0 mg at months 6, 9, and 12, respectively. The most frequently reported adverse events were nausea (n = 93, 24.0 percent) and constipation (n = 75, 19.3 percent). The analgesic effects of OROS® hydromorphone, assessed using the Brief Pain Inventory, were maintained throughout the extension. At 12 months, 72.4 percent of patients and 75.9 percent of investigators rated overall treatment as good, very good, or excellent.
Conclusions: Once-daily OROS® hydromorphone is an osmotically driven, controlled-release preparation that may be particularly well suited to long-term use, because it provides consistent plasma concentrations and sustained around-the-clock analgesia. In this study, the benefits of OROS® hydromorphone attained in short-term studies were maintained in the long-term when daily administration was continued.
References
Harstall C, Ospina M: How prevalent is chronic pain? Pain: Clinical Updates. 2003; XI(2): 1-4.
Breivik H, Collett B, Ventafridda V, et al.: Survey of chronic pain in Europe: Prevalence, impact on daily life, and treatment. Eur J Pain. 2006; 10(4): 287-333.
Chronic pain in America: Roadblocks to relief, 1999. Available at: www.ampainsoc.org/links/roadblocks/. Accessed May 31, 2006.
Lazarus H, Neumann CJ: Assessing undertreatment of pain: The patients’ perspectives. J Pharm Care Pain Symptom Control. 2001; 9(4): 5-34.
Croft PR, Macfarlane GJ, Papageorgiou AC, et al.: Outcome of low back pain in general practice: A prospective study. BMJ. 1998; 316(7141): 1356-1359.
Angst MS, Drover DR, Lotsch J, et al.: Pharmacodynamics of orally administered sustained-release hydromorphone in humans. Anesthesiology. 2001; 94(1): 63-73.
Drover DR, Angst MS, Valle M, et al.: Input characteristics and bioavailability after administration of immediate and a new extended-release formulation of hydromorphone in healthy volunteers. Anesthesiology. 2002; 97(4): 827-836.
Hale M, Tudor IC, Khanna S, et al.: Efficacy and tolerability of once-daily OROS hydromorphone and twice-daily extendedrelease oxycodone in patients with chronic, moderate to severe osteoarthritis pain: Results of a 6-week, randomized, openlabel, noninferiority analysis. Clin Ther. 2007; 29(5): 874-888.
Wallace M, Rauck RL, Moulin D, et al.: Conversion from standard opioid therapy to once-daily oral, extended-release hydromorphone in patients with chronic cancer pain. J Int Med Res. 2007; 36(2): 343-352.
Wallace M, Rauck RL, Moulin D, et al.: Once-daily OROS hydromorphone for the management of chronic nonmalignant pain: A dose-conversion and titration study. Int J Clin Pract. 2007; 61(10): 1671-1676.
Daut RL, Cleeland CS, Flanery RC: Development of the Wisconsin Brief Pain Questionnaire to assess pain in cancer and other diseases. Pain. 1983; 17(2): 197-210.
Eisenberg E, McNicol ED, Carr DB: Efficacy and safety of opioid agonists in the treatment of neuropathic pain of nonmalignant origin: Systematic review and meta analysis of randomized controlled trials. JAMA. 2005; 293(24): 3043-3052.
Roth SH, Fleischmann RM, Burch FX, et al.: Around-theclock, controlled-release oxycodone therapy for osteoarthritisrelated pain: Placebo-controlled trial and long-term evaluation. Arch Intern Med. 2000; 160(6): 853-860.
McIlwain H, Ahdieh H: Safety, tolerability, and effectiveness of oxymorphone extended release for moderate to severe osteoarthritis pain: A one-year study. Am J Ther. 2005; 12(2): 106-112.
Allan L, Richarz U, Simpson K, et al.: Transdermal fentanyl versus sustained-release oral morphine in strong-opioid naive patients with chronic low back pain. Spine. 2005; 30(22): 2484-2490.
Mitra S: Opioid-induced hyperalgesia: Pathophysiology and clinical implications. J Opioid Manag. 2008; 4(3): 123-130.
Chu LF, Angst MS, Clark D: Opioid-induced hyperalgesia in humans: Molecular mechanisms and clinical considerations. Clin J Pain. 2008; 24(6): 479-496.
Cherny N: New strategies in opioid therapy for cancer pain. J Oncol Manag. 2000; 9(1): 8-15.
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