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February 08, 2000; 54 (3) Articles

Intravenous lidocaine in central pain

A double-blind, placebo-controlled, psychophysical study

N. Attal, V. Gaudé, L. Brasseur, M. Dupuy, F. Guirimand, F. Parker, D. Bouhassira
First published February 8, 2000, DOI: https://doi.org/10.1212/WNL.54.3.564
N. Attal
MD, PhD
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V. Gaudé
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L. Brasseur
MD
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M. Dupuy
MD
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F. Guirimand
MD, PhD
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F. Parker
MD
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D. Bouhassira
MD, PhD
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Citation
Intravenous lidocaine in central pain
A double-blind, placebo-controlled, psychophysical study
N. Attal, V. Gaudé, L. Brasseur, M. Dupuy, F. Guirimand, F. Parker, D. Bouhassira
Neurology Feb 2000, 54 (3) 564; DOI: 10.1212/WNL.54.3.564

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Abstract

Objective: To investigate the effects of systemic administration of lidocaine on different components of neuropathic central pains by quantitative sensory testing.

Methods: The efficacy of systemic lidocaine (5 mg/kg IV over 30 minutes) was evaluated in a double-blind, placebo-controlled, and cross-over fashion, on both spontaneous ongoing pain and evoked pains (allodynia and hyperalgesia) in 16 patients with chronic poststroke (n = 6) or spinal cord injury (n = 10) related pain.

Results: Lidocaine was significantly superior to the placebo (saline) in reducing the intensity of spontaneous ongoing pain for up to 45 minutes after the injection: 10 of 16 patients (62.5%) receiving lidocaine showed a significant reduction in spontaneous pain, whereas only six patients showed this after the placebo. Lidocaine also significantly reduced the intensity of brush-induced allodynia and mechanical hyperalgesia, but was no better than the placebo against thermal allodynia and hyperalgesia. In general, the side effects were moderate and consisted mainly of lightheadedness (44%).

Conclusions: Systemic lidocaine can induce a significant and selective reduction of several components of pain caused by CNS injuries. The observed preferential antihyperalgesic and antiallodynic effects of this drug suggest a selective central action on the mechanisms underlying these evoked pains.

  • Received July 8, 1999.
  • Accepted August 31, 1999.
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  • Article
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