A Pilot Study
- 1 December 1992
- journal article
- research article
- Published by Wolters Kluwer Health in The Clinical Journal of Pain
- Vol. 8 (4) , 338-345
- https://doi.org/10.1097/00002508-199212000-00008
Abstract
Objective To assess the efficacy of acute intrathecai (i.t.) baciofen on chronic, dysesthetic, and spasm-related pain (SRP) among patients with spinal spasticity [i.e., multiple sclerosis (MS), spinal cord injury (SCI), transverse myelitis (TMy)]. Design Double-blind, randomized, and placebo (vehicle) controlled trials (n = 7), and nonrandomized, nonblinded trials (n = 2). Setting In-patient program at Samaritan Rehabilitation Institute, Phoenix, Arizona, U.S.A. Patients MS (n = 4), spinal cord compression (n = 1), and TMy (n = 2) in the double-blind trial, and SCI (n = 2) in the nonblinded trial; all had chronic spinal lesions and function-limiting spasticity refractory to oral medications, including baciofen (p.o). Interventions i.t. baciofen (50 μg) in 1 ml preservative-free normal saline into the L1–2 interspace. Outcome Measures Electromyographic (EMG) activity; intravesical and intraurethral pressures; Ashworth Scale and tendon response values; visual analog scales for describing dysesthetic pain intensity; and threshold/EMG relationships after controlled pinch as an indication of nociceptive pain. Results i.t. baciofen (a) caused marked reduction of segmental reflexes before suppression of intersegmental reflexes; (b) significantly suppressed dysesthetic pain and SRP with temporal dissociation; and (3) did not influence pinch-induced and musculoskeletal (low back) pain. Conclusions The suppressive action of i.t. baciofen on spontaneous and evoked (allodynia) dysesthetic pain suggests that a dysfunctional spinal γ-aminobutyric acidB receptor system, including functional supersensitivity, is associated with the phenomenon of central pain among patients with spinal lesions. Temporal dissociation regarding the action on dysesthetic pain and SRP suggests that disparate central mechanisms subserve the two clinical states.Keywords
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