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Topiramate in painful diabetic polyneuropathy: findings from three double‐blind placebo‐controlled trials
Author(s) -
Thienel U.,
Neto W.,
Schwabe S. K.,
Vijapurkar U.
Publication year - 2004
Publication title -
acta neurologica scandinavica
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.967
H-Index - 95
eISSN - 1600-0404
pISSN - 0001-6314
DOI - 10.1111/j.1600-0404.2004.00338.x
Subject(s) - topiramate , placebo , medicine , tolerability , adverse effect , neuropathic pain , anesthesia , clinical trial , visual analogue scale , polyneuropathy , randomized controlled trial , epilepsy , psychiatry , alternative medicine , pathology
Objectives – To evaluate the efficacy and tolerability of topiramate in patients with painful diabetic polyneuropathy. Materials and methods – Patients with moderate to extreme pain (0–4 Categorical Pain Scale score ≥ 2) were randomized to placebo or topiramate (100, 200, or 400 mg/day) in three similar double‐blind trials. The primary efficacy analysis was pain reduction from final visit to baseline in the 100‐mm Visual Analog Scale (VAS) for the intent‐to‐treat populations. Results – After 18–22 weeks of double‐blind treatment, pain reductions were numerically greater with topiramate in two studies but differences between topiramate and placebo in VAS scores or in the secondary efficacy endpoints did not reach statistical significance in any of the three studies. Across all studies, 24% of topiramate‐treated patients and 8% of placebo‐treated patients discontinued due to adverse events; groups did not differ in the occurrence of serious adverse events. Conclusion – These studies did not find topiramate to be significantly more effective than placebo in reducing pain scores in patients with painful diabetic polyneuropathy. Several design features may have precluded the studies from having sufficient sensitivity to differentiate effective and ineffective treatments. The study design and results are instructive for other investigators designing future clinical studies in neuropathic pain.