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Duloxetine for Central Pain in MS

A Randomized Placebo-Controlled Trial of Duloxetine for Central Pain in Multiple Sclerosis

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Year of Publication: 2015

Authors: Theodore R. Brown, April Slee

Journal: International Journal of MS Care

Citation: Brown TR, Slee A. A Randomized Placebo-Controlled Trial of Duloxetine for Central Pain in Multiple Sclerosis. Int J MS Care. 2015;17:83-89. DOI: 10.7224/1537-2073.2014-001

Link: http://dx.doi.org/10.7224/1537-2073.2014-001

PDF: https://pmc.ncbi.nlm.nih.gov/articles/PM...073-17-2-83.pdf

Clinical Question

Does duloxetine, a serotonin-norepinephrine reuptake inhibitor (SNRI), provide effective pain relief for central pain in patients with multiple sclerosis compared to placebo?

Bottom Line

Among MS patients who completed 6 weeks of treatment, duloxetine 60 mg daily significantly reduced both worst pain (29% reduction vs 12% placebo, P=0.016) and average pain (39% reduction vs 10% placebo, P=0.002). However, tolerability was a significant issue with 22% of duloxetine patients discontinuing due to adverse effects versus 10% of placebo patients. The findings suggest duloxetine has a direct pain-relieving effect in MS and may be considered as a second-line therapeutic option, though not all patients will tolerate the medication.

Major Points

  • First randomized controlled trial specifically examining duloxetine for MS-related central pain with detailed pain diary outcomes
  • Significant reduction in both worst pain (29%) and average pain (39%) with duloxetine versus placebo at 6 weeks
  • Pain relief evident as early as 2 weeks for average pain and 4 weeks for worst pain
  • Clinically meaningful pain reduction (>30% improvement) achieved in 44% of duloxetine patients vs 5% of placebo for average pain
  • Tolerability concerns limit clinical utility - 22% discontinuation rate in duloxetine group due to adverse effects
  • No significant improvements in mood, sleep quality, or quality of life measures, suggesting direct analgesic effect rather than indirect effects through mood improvement
  • Study supports duloxetine as second-line agent for MS pain, after anticonvulsants or tricyclic antidepressants
  • Daily pain diaries used to capture real-time patient-reported outcomes
  • Rescue medication (NSAIDs/acetaminophen) allowed and tracked
  • Small sample size (38 patients) due to slow recruitment and funding limitations

Design

Study Type: Parallel-group, double-blind, randomized, placebo-controlled trial

Randomization: 1

Blinding: Double-blind. Treating physician and examining research coordinators blinded to treatment allocation until end of trial. Randomization performed at clinical research pharmacy

Enrollment Period: Not specified

Follow-up Duration: 6 weeks acute therapy phase plus 1 week taper period (7 weeks total treatment), with follow-up phone call 2 weeks after final visit

Centers: 1

Countries: United States

Sample Size: 38

Analysis: Primary analysis on per-protocol population (completed 6 weeks with good adherence). Intent-to-treat sensitivity analyses performed using two imputation strategies: (1) imputing placebo mean for missing data, (2) imputing worst observed value. Between-group comparisons using independent samples t-test. Fisher exact test for categorical variables and responder rates (>30% pain reduction). No adjustment for multiple comparisons beyond primary outcome. Powered for 54 patients based on 1.75 point difference on 0-10 scale with SD 2.1 and 85% power at 5% significance

Inclusion Criteria

  • MS diagnosis based on McDonald or Poser criteria at least 3 months prior to screening
  • Age >18 years
  • No MS exacerbation for 90 days prior to screening
  • No change in disease-modifying therapy for 90 days prior to screening
  • Daily pain attributed to MS by treating physician
  • Pain present for minimum of 2 months prior to screening
  • Worst pain score ≥4 on 11-point (0-10) Likert scale on majority of recorded days
  • At least 5 valid daily pain diary scores required
  • Pain clearly differentiated from non-MS causes (diabetic neuropathy, peripheral vascular disease, arthritis, musculoskeletal conditions, chronic headache, visceral pain excluded)

Exclusion Criteria

  • Current or historical diagnosis of mania, bipolar disorder, or psychosis
  • Concomitant use of MAO inhibitors, SSRIs, SNRIs, tryptophan, St. John's wort
  • Use of medicinal marijuana
  • Use of as-needed analgesic medication (except study-related rescue therapy)
  • Regularly scheduled opiates or anticonvulsants were allowed
  • Uncontrolled narrow-angle glaucoma
  • Depression with suicidality
  • Alcohol abuse
  • Chronic hepatic insufficiency or ALT/AST >2× upper limit of normal
  • Renal insufficiency (creatinine clearance <30 mL/min or serum creatinine >1.9)
  • Uncontrolled hypertension (SBP >180, DBP >105)
  • Breast-feeding or pregnancy in females
  • Any other serious and/or unstable medical condition

Baseline Characteristics

CharacteristicDuloxetine Per-ProtocolPlacebo Per-Protocol
Age (years)54.71±9.9756.33±11.23
Female sex78.6%72.2%
MS type - RRMS71.4%61.1%
MS type - PPMS21.4%16.7%
MS type - PRMS/SPMS7.1%22.2%
Years since MS diagnosis13.68±9.8713.78±7.49
Disease-modifying drug use92.9%55.6%
EDSS score5.07±1.765.00±1.67
Pain location - Legs64.3%55.6%
Pain location - Arms28.6%27.8%
Pain location - Trunk21.4%38.9%
Pain location - Pelvis14.3%11.1%
Baseline pain medications - Any92.9%100%
Baseline pain medications - Anticonvulsant35.7%38.9%
Baseline pain medications - NSAID50.0%33.3%
Worst pain score6.74±1.616.36±1.57
Average pain score4.66±1.784.36±1.51
Sleep score3.70±2.044.58±1.89
Number of rescue medications3.29±3.583.75±2.78
Beck Depression Inventory8.21±5.7912.89±8.59
SF-36 Physical component32.05±7.5736.63±7.49
SF-36 Mental component54.21±8.8547.75±11.74

Arms

FieldControlDuloxetine
InterventionMatched placebo capsules administered three times weekly (mimicking duloxetine dosing schedule) for 7 weeks. Rescue medication allowed: ibuprofen up to 2400 mg/day (12 tablets of 200 mg) provided by research pharmacy; patients unable to tolerate ibuprofen could substitute acetaminophen up to 2000 mg/day (6 tablets of 325 mg). No as-needed analgesic medication or medicinal marijuana allowed from 7 days prior to baseline until after acute phase (week 6)Duloxetine 30 mg orally daily (morning dose with food) for 1 week, then 60 mg daily for 5 weeks, then 30 mg daily for 1 week taper to limit discontinuation-emergent adverse events. Same rescue medication protocol as placebo: ibuprofen up to 2400 mg/day or acetaminophen up to 2000 mg/day if ibuprofen not tolerated. No as-needed analgesic medication or medicinal marijuana allowed from 7 days prior to baseline until after acute phase (week 6)
Duration7 weeks total (6 weeks acute phase + 1 week for observation)7 weeks total (1 week 30mg + 5 weeks 60mg + 1 week 30mg taper)

Outcomes

OutcomeTypeControlInterventionHR / OR / RRP-value
Percent change in worst pain score from baseline to week 6, recorded daily on pain diary using 0-10 visual analogue scale in per-protocol populationPrimary0.016
Percent change in average pain score from baseline to week 6 | Duloxetine: Mean reduction 38.5% (SD 29.1%), absolute change -1.7 points; Placebo: Mean reduction 10.4% (SD 18.9%)Secondary0.002
Proportion with >30% reduction in worst pain at week 6 | Duloxetine: 33%; Placebo: 10%Secondary0.117 (not significant)
Proportion with >30% reduction in average pain at week 6 | Duloxetine: 44%; Placebo: 5%Secondary0.007
Change in sleep score at week 6 | Duloxetine: Slight decline; Placebo: Slight declineSecondaryNot significant
Change in Beck Depression Inventory at week 6 | Duloxetine: Slight improvement; Placebo: Slight improvementSecondaryNot significant
Change in SF-36 quality of life at week 6 | Duloxetine: Slight improvement; Placebo: Slight improvementSecondaryNot significant
Change in rescue medication use at week 6 | Duloxetine: Reduced by 1.9 medications from baseline; Placebo: Reduced by 0.7 medications from baselineSecondaryNot significant
Subject global impression at week 6 | Duloxetine: Mean 4.8; Placebo: Mean 3.9Secondary0.074 (approached significance)
ITT analysis - worst pain (imputing placebo mean for missing data) | Duloxetine: Remained significant; Placebo: ReferenceSecondary0.0204
ITT analysis - worst pain (imputing worst observed value +40.1) | Duloxetine: Not significant; Placebo: ReferenceSecondaryNot significant
ITT analysis - average pain (both imputation strategies) | Duloxetine: Remained significant; Placebo: ReferenceSecondary0.0043
Early discontinuation - duloxetineAdverseDuloxetine: 4 patients (22%): (1) worsening idiopathic thrombocytopenic purpura-related thrombocytopenia, (1) blurred vision and nausea, (1) vertigo and dizziness, (1) worsening depression; Placebo: 2 patients (10%): (1) headache, (1) stopped medication during final week but continued participationNot reported
NauseaAdverseDuloxetine: 2 patients; Placebo: Not reportedNot reported
DizzinessAdverseDuloxetine: 2 patients; Placebo: Not reportedNot reported
HeadacheAdverseDuloxetine: 2 patients; Placebo: 2 patientsNot reported
Increased fatigueAdverseDuloxetine: 2 patients; Placebo: Not reportedNot reported
ConstipationAdverseDuloxetine: 2 patients; Placebo: Not reportedNot reported
Urinary incontinence or hesitancyAdverseDuloxetine: 3 patients; Placebo: Not reportedNot reported
FallsAdverseDuloxetine: 3 patients (none suspected related to study drug); Placebo: 3 patients (none suspected related to study drug)Not reported
ThrombocytopeniaAdverseDuloxetine: 1 patient (history of idiopathic thrombocytopenic purpura); Placebo: 1 patientNot reported
Liver function test abnormalitiesAdverseDuloxetine: 0 patients; Placebo: 1 patientNot reported
Serious adverse eventsAdverseDuloxetine: 0 patients; Placebo: 0 patientsNot applicable

Subgroup Analysis

Not performed in this study

Criticisms

  • Small sample size (38 patients) - less than target enrollment of 54 patients due to slow recruitment and funding limitations, reducing statistical power
  • Short treatment duration (only 6 weeks of acute therapy) - may not be sufficient to assess longer-term efficacy or antidepressant effects which typically require 6-8 weeks
  • High dropout rate in duloxetine group (22%) due to adverse effects limits clinical utility and affects intent-to-treat analysis
  • Pain etiology verification challenging - efforts made to exclude non-neurogenic causes but cannot guarantee all pain was truly MS-related central neuropathic pain
  • Missing data from early terminators affects robustness - worst pain outcome became non-significant with worst-case imputation
  • Single-center study limits generalizability
  • No active comparator - comparison only to placebo, not to other standard treatments like anticonvulsants or tricyclic antidepressants
  • Excluded patients already on SSRIs, SNRIs, or MAO inhibitors - may have excluded clinically relevant population
  • Study excluded patients with low baseline pain (<4/10) - benefit-to-risk ratio may be less favorable in milder pain
  • No long-term follow-up to assess durability of pain relief or late-emerging adverse effects
  • Lack of blinding for pain diary completion (patient-reported) - though outcome assessors were blinded
  • Use of rescue medication allowed - may have confounded results, though usage was tracked
  • No correction for multiple comparisons beyond primary outcome - secondary outcomes should be considered hypothesis-generating

Funding

Independent medical grant from Lilly Inc (manufacturer of duloxetine/Cymbalta)

Based on: Duloxetine for Central Pain in MS (International Journal of MS Care, 2015)

Authors: Theodore R. Brown, April Slee

Citation: Brown TR, Slee A. A Randomized Placebo-Controlled Trial of Duloxetine for Central Pain in Multiple Sclerosis. Int J MS Care. 2015;17:83-89. DOI: 10.7224/1537-2073.2014-001

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