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ABSTRACT
Objective
Concerns regarding the efficacy, toxicity, tolerance, dependence, and abuse
of opioids have limited their use for patients with chronic spine pain. In our
previous study of rheumatology clinic patients, opioid analgesics were found to
be highly effective, produced only mild side effects, and had few instances of
opioid abuse. The purpose of this study was to replicate our previous study in
another large cohort of patients with nonmalignant pain due to well-defined
spinal diseases.
Method
Opioid use was studied in 230 orthopedics spine clinic patients by retrospective
analysis of prescriptions for 3 years and cross-sectional analysis of efficacy
and toxicity by patient interviews. Opioid use and stability of the daily dose
over 3 years were derived from computerized pharmacy records. Medical records,
operative reports, and radiographic studies were reviewed to determine the
reason for dosage escalations and to detect instances of abuse or addiction
behaviors. Patients were interviewed to determine the efficacy, frequency, and
types of side effects and instances of obtaining opioids from sources outside
the Veterans Affairs system.
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Results
Opioids were prescribed for 152 of the 230 patients, for <3 months (short-term [STO])
in 94, 3 months (long-term [LTO]) in 58, and none in 72 (no opioid [NTO]).
Medications prescribed were codeine, oxycodone, propoxyphene, tramadol,
morphine, meperidine, fentanyl, or hydroxycodone, either alone or in
combination. Interviews were completed in 72 STO, 50 LTO, and 45 NTO patients.
Pain severity (0-10 scale) was not different in patients with different spinal
pathologies. Opioids significantly reduced the back pain severity score from 8.3
± 1.5 to 4.5 ± 2.2 (mean ± SD). Mild side effects (most commonly, constipation
and sedation) were reported by 58% of the opioid-treated patients but rarely
caused them to stop taking the medication. There was no significant increase
from the mean ± SD initial opioid dosage of 5.0 ± 12.2 30-mg codeine equivalents
per day (30 mg oral codeine = 5 mg oral morphine) to the mean peak dosage of 7.9
± 12.5 and the mean recent dosage of 4.3 ± 6.3, suggesting that tolerance to
opioid analgesia did not appear to occur in these patients. Dosage escalations
of >2 30-mg codeine equivalents occurred 19 times in 17 LTO patients and was due
to worsening of the underlying painful condition, complications of spine
surgery, or unrelated surgical or medical problems in all but 3 of them (5%).
These 3 patients also displayed other abuse behaviors. Abuse behaviors were not
more frequent in those with or without a history of abuse/addiction.
Conclusions
This study provides data on the efficacy, toxicity, tolerance, and abuse or
addiction behaviors with opioid therapy in a large cohort of patients in an
orthopedics spine clinic. The results provide objective data from patients with
well-defined spine diagnoses to challenge the position that opioid treatment is
inappropriate for chronic nonmalignant pain. This study provides clinical
evidence to support and protect physicians treating patients with chronic
musculoskeletal diseases, who may be reluctant to prescribe opioids because of
possible sanctions from regulatory agencies. More important, it will benefit
patients by permitting them to receive these effective, safe medications.
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