• Pain Med · Apr 2012

    Review Meta Analysis Comparative Study

    Placebo response changes depending on the neuropathic pain syndrome: results of a systematic review and meta-analysis.

    • M Soledad Cepeda, Jesse A Berlin, C Yuying Gao, Frank Wiegand, and D Russell Wada.
    • Janssen Research and Development, L.L.C., Titusville, New Jersey 08560, USA. scepeda@its.jnj.com
    • Pain Med. 2012 Apr 1;13(4):575-95.

    ObjectiveTo compare placebo responses in neuropathic pain syndromes.DesignSystematic literature review and meta-analysis.Setting And PatientsRandomized placebo-controlled trials assessing pain intensity or pain relief in any neuropathic pain syndrome published since 1995 with ≥5days follow-up.InterventionsPlacebo response.Outcome MeasuresPain intensity and responder rates (proportion reporting ≥50% pain relief). Meta-regression models were built.ResultsNinety-four studies (N=5,317) were included in the pain intensity analysis; 47 studies (N=3,087) were included in the responder analysis. After controlling for potential confounders (e.g., subject characteristics, study design characteristics), the placebo response was found to be large and varied with the pain syndrome. Compared with diabetic neuropathic/polyneuropathic pain (DPN), the placebo response for a decline in pain intensity and responder rate was smaller in trials that assessed central pain and postherpetic neuralgia (PHN) and larger in trials that assessed HIV pain. The model-predicted mean decrease (95% confidence interval [CI]) from baseline in pain intensity (0-10 scale) was as follows: DPN, 1.45 (1.35 to 1.55); PHN, 1.16 (1.03 to 1.29); central pain, 0.44 (-0.41 to 1.30); HIV pain, 1.82 (1.51 to 2.12). The predicted responder rates (95% CI) were as follows: DPN, 20% (14.6 to 25.8); PHN, 11.5% (8.4 to 14.5); central pain, 7.2% (2.1 to 12.3); HIV pain, 42.8% (34.9 to 50.7). The type of treatment in the active arm also influenced the placebo response.ConclusionsPlacebo response is influenced by the pain syndrome evaluated. These differences should be considered when evaluating novel compounds for the treatment of neuropathic pain conditions.Wiley Periodicals, Inc.

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