Traumatic Brain Injury Clinical Trial
Official title:
Partial Blocks of Rectus Femoris and Soleus With Botulinum Toxin Type A to Improve Gait in Hemiparesis. A Randomized Multicenter Placebo-controlled Trial
The most common motor deficiency after stroke or traumatic brain injury is hemiparesis. Most
hemiparetic patients recover walking, but rarely with a speed permitting easy ambulation
outdoors with family or friends. One of the mechanisms of gait impairment in hemiparesis is
insufficient active hip flexion during swing phase, which leads to insufficient ground
clearing at swing phase, with associated gait slowness and risks of fall.
The main hypothesis behind the present study is that insufficient hip flexion during
hemiparetic gait is partly due to overactivity of rectus femoris. Focal treatment of lower
limb muscle overactivity using botulinum toxin has not been demonstrated to increase walking
speed in hemiparesis as yet. However, most studies have focused distally, on improving foot
dorsiflexion only. The purpose of this study is to compare the effects of botulinum toxin
injection and placebo in rectus femoris (RF) + plantar flexors versus plantar flexors only.
Randomized, double blind, parallel-group study in chronic, non-evolutive brain damaged
patients (>6 months since stroke or brain trauma) and ambulating at <1.3 m/sec at maximal
speed barefoot (AT10) Group 1: 150U (x 7.5 ml) placebo Sol + 150U (x 7.5 ml) placebo RF +
100U (5ml) placebo distributed between tibialis posterior, FHL (flexor hallucis longus), FCB
(flexor digitorum brevis), gastrocnemius muscles or peroneus longus, based upon investigator
clinical judgment.
Group 2: 150U (x 7.5 ml) Xeomin® 20U/ml Sol + 150U (x 7.5 ml) placebo RF + 100U (5ml)
Xeomin® distributed between tibialis posterior, FHL (flexor hallucis longus), FCB (flexor
digitorum brevis), gastrocnemius muscles or peroneus longus, based upon investigator
clinical judgment.
Group 3: 150U (x 7.5 ml) Xeomin® 20U/ml Sol + 150U (x 7.5 ml) Xeomin® 20U/ml RF + 100U (5ml)
Xeomin® distributed between tibialis posterior, FHL (flexor hallucis longus), FCB (flexor
digitorum brevis), gastrocnemius muscles or peroneus longus, based upon investigator
clinical judgment.
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