Cerebrospinal fluid levels of opioid peptides in fibromyalgia and chronic low back pain

The mechanism(s) of nociceptive dysfunction and potential roles of opioid neurotransmitters are unresolved in the chronic pain syndromes of fibromyalgia and chronic low back pain. History and physical examinations, tender point examinations, and questionnaires were used to identify 14 fibromyalgia,...

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Bibliographic Details
Published in:BMC musculoskeletal disorders 2004-12, Vol.5 (1), p.48-48, Article 48
Main Authors: Baraniuk, James N, Whalen, Gail, Cunningham, Jill, Clauw, Daniel J
Format: Article
Language:English
Subjects:
Adult
Aged
Chronic Disease
Enkephalin, Methionine - analogs & derivatives
Enkephalin, Methionine - cerebrospinal fluid
Fatigue Syndrome, Chronic - complications
Female
Fibromyalgia - cerebrospinal fluid
Fibromyalgia - complications
Humans
Low Back Pain - cerebrospinal fluid
Male
Middle Aged
Nociceptin
Opioid Peptides - cerebrospinal fluid
Pain - physiopathology
Pain Measurement
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Summary:The mechanism(s) of nociceptive dysfunction and potential roles of opioid neurotransmitters are unresolved in the chronic pain syndromes of fibromyalgia and chronic low back pain. History and physical examinations, tender point examinations, and questionnaires were used to identify 14 fibromyalgia, 10 chronic low back pain and 6 normal control subjects. Lumbar punctures were performed. Met-enkephalin-Arg6-Phe7 (MEAP) and nociceptin immunoreactive materials were measured in the cerebrospinal fluid by radioimmunoassays. Fibromyalgia (117.6 pg/ml; 85.9 to 149.4; mean, 95% C.I.; p = 0.009) and low back pain (92.3 pg/ml; 56.9 to 127.7; p = 0.049) groups had significantly higher MEAP than the normal control group (35.7 pg/ml; 15.0 to 56.5). MEAP was inversely correlated to systemic pain thresholds. Nociceptin was not different between groups. Systemic Complaints questionnaire responses were significantly ranked as fibromyalgia > back pain > normal. SF-36 domains demonstrated severe disability for the low back pain group, intermediate results in fibromyalgia, and high function in the normal group. Fibromyalgia was distinguished by higher cerebrospinal fluid MEAP, systemic complaints, and manual tender points; intermediate SF-36 scores; and lower pain thresholds compared to the low back pain and normal groups. MEAP and systemic pain thresholds were inversely correlated in low back pain subjects. Central nervous system opioid dysfunction may contribute to pain in fibromyalgia.
ISSN:1471-2474
1471-2474
DOI:10.1186/1471-2474-5-48