Analgesic tolerance without demonstrable opioid-induced hyperalgesia: A double-blinded, randomized, placebo-controlled trial of sustained-release morphine for treatment of chronic nonradicular low-back pain
After 1month of oral morphine therapy, chronic low-back pain patients developed tolerance but not opioid-induced hyperalgesia. Improvements in pain and functional ability were observed. Although often successful in acute settings, long-term use of opioid pain medications may be accompanied by waning...
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Published in | Pain (Amsterdam) Vol. 153; no. 8; pp. 1583 - 1592 |
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Main Authors | , , , , , , , , |
Format | Journal Article |
Language | English |
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Philadelphia, PA
Elsevier B.V
01.08.2012
Elsevier |
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Abstract | After 1month of oral morphine therapy, chronic low-back pain patients developed tolerance but not opioid-induced hyperalgesia. Improvements in pain and functional ability were observed.
Although often successful in acute settings, long-term use of opioid pain medications may be accompanied by waning levels of analgesic response not readily attributable to advancing underlying disease, necessitating dose escalation to attain pain relief. Analgesic tolerance, and more recently opioid-induced hyperalgesia, have been invoked to explain such declines in opioid effectiveness over time. Because both phenomena result in inadequate analgesia, they are difficult to distinguish in a clinical setting. Patients with otherwise uncomplicated low-back pain were titrated to comfort or dose-limiting side effects in a prospective, randomized, double-blind, placebo-controlled clinical trial using sustained-release morphine or weight-matched placebo capsules for 1month. A total of 103 patients completed the study, with an average end titration dose of 78mgmorphine/d. After 1month, the morphine-treated patients developed tolerance to the analgesic effects of remifentanil, but did not develop opioid-induced hyperalgesia. On average, these patients experienced a 42% reduction in analgesic potency. The morphine-treated patients experienced clinically relevant improvements in pain relief, as shown by a 44% reduction in average visual analogue scale pain levels and a 31% improvement in functional ability. The differences in visual analogue scale pain levels (P=.003) and self-reported disability (P=.03) between both treatment groups were statistically significant. After 1month of oral morphine therapy, patients with chronic low-back pain developed tolerance but not opioid-induced hyperalgesia. Improvements in pain and functional ability were observed. |
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AbstractList | Although often successful in acute settings, long-term use of opioid pain medications may be accompanied by waning levels of analgesic response not readily attributable to advancing underlying disease, necessitating dose escalation to attain pain relief. Analgesic tolerance, and more recently opioid-induced hyperalgesia, have been invoked to explain such declines in opioid effectiveness over time. Because both phenomena result in inadequate analgesia, they are difficult to distinguish in a clinical setting. Patients with otherwise uncomplicated low-back pain were titrated to comfort or dose-limiting side effects in a prospective, randomized, double-blind, placebo-controlled clinical trial using sustained-release morphine or weight-matched placebo capsules for 1 month. A total of 103 patients completed the study, with an average end titration dose of 78 mg morphine/d. After 1 month, the morphine-treated patients developed tolerance to the analgesic effects of remifentanil, but did not develop opioid-induced hyperalgesia. On average, these patients experienced a 42% reduction in analgesic potency. The morphine-treated patients experienced clinically relevant improvements in pain relief, as shown by a 44% reduction in average visual analogue scale pain levels and a 31% improvement in functional ability. The differences in visual analogue scale pain levels (P = .003) and self-reported disability (P = .03) between both treatment groups were statistically significant. After 1 month of oral morphine therapy, patients with chronic low-back pain developed tolerance but not opioid-induced hyperalgesia. Improvements in pain and functional ability were observed. After 1month of oral morphine therapy, chronic low-back pain patients developed tolerance but not opioid-induced hyperalgesia. Improvements in pain and functional ability were observed. Although often successful in acute settings, long-term use of opioid pain medications may be accompanied by waning levels of analgesic response not readily attributable to advancing underlying disease, necessitating dose escalation to attain pain relief. Analgesic tolerance, and more recently opioid-induced hyperalgesia, have been invoked to explain such declines in opioid effectiveness over time. Because both phenomena result in inadequate analgesia, they are difficult to distinguish in a clinical setting. Patients with otherwise uncomplicated low-back pain were titrated to comfort or dose-limiting side effects in a prospective, randomized, double-blind, placebo-controlled clinical trial using sustained-release morphine or weight-matched placebo capsules for 1month. A total of 103 patients completed the study, with an average end titration dose of 78mgmorphine/d. After 1month, the morphine-treated patients developed tolerance to the analgesic effects of remifentanil, but did not develop opioid-induced hyperalgesia. On average, these patients experienced a 42% reduction in analgesic potency. The morphine-treated patients experienced clinically relevant improvements in pain relief, as shown by a 44% reduction in average visual analogue scale pain levels and a 31% improvement in functional ability. The differences in visual analogue scale pain levels (P=.003) and self-reported disability (P=.03) between both treatment groups were statistically significant. After 1month of oral morphine therapy, patients with chronic low-back pain developed tolerance but not opioid-induced hyperalgesia. Improvements in pain and functional ability were observed. |
Author | D’Arcy, Nicole Clark, J. David Young, Chelsea Anne Clemenson, Anna Marie Zamora, Abigail Kathleen Chu, Larry F. Kim, Julie Eunwoo Brady, Caitlin Angst, Martin S. |
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Keywords | Analgesic tolerance Opioid-induced hyperalgesia Low-back pain Nonradicular Chronic opioid therapy Human Lumbar spine Low back pain Diseases of the osteoarticular system Tolerance Morphine Spine disease Long term Hyperalgesia Prospective Analgesia Analgesic Pain Treatment Placebo Rachialgia Release |
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Snippet | After 1month of oral morphine therapy, chronic low-back pain patients developed tolerance but not opioid-induced hyperalgesia. Improvements in pain and... Although often successful in acute settings, long-term use of opioid pain medications may be accompanied by waning levels of analgesic response not readily... |
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SubjectTerms | Adolescent Adult Aged Analgesic tolerance Analgesics Biological and medical sciences Chronic opioid therapy Delayed-Action Preparations - adverse effects Delayed-Action Preparations - therapeutic use Double-Blind Method Drug Tolerance Female Humans Hyperalgesia - chemically induced Hyperalgesia - diagnosis Low Back Pain - complications Low Back Pain - diagnosis Low Back Pain - drug therapy Low-back pain Male Medical sciences Middle Aged Morphine - adverse effects Morphine - therapeutic use Nervous system (semeiology, syndromes) Nervous system as a whole Neurology Neuropharmacology Nonradicular Opioid-induced hyperalgesia Opioid-Related Disorders - diagnosis Opioid-Related Disorders - etiology Pain Measurement - drug effects Pharmacology. Drug treatments Placebo Effect Treatment Outcome Young Adult |
Title | Analgesic tolerance without demonstrable opioid-induced hyperalgesia: A double-blinded, randomized, placebo-controlled trial of sustained-release morphine for treatment of chronic nonradicular low-back pain |
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