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Clinical Trial Summary

The aim of the study was to compare Dysport treatment results (as assessed by Modified Ashworth Scale (MAS) in the elbow joint 4 weeks post treatment) following two treatment techniques: the current clinical practice injection technique using high-concentration dilution (300 U/mL Dysport) versus the neuromuscular junction (NMJ)-targeted injection technique using low-concentration dilution (100 U/mL Dysport). The hypothesis was that one high-volume, low-concentration injection located centrally in the area/band of the NMJ zones would be as effective as the technique used in current medical practice.


Clinical Trial Description

This was a randomised, evaluator-blinded, comparative, parallel group, multicentre study, conducted in four countries (Denmark, Finland, Norway and Sweden). For each subject, the primary efficacy assessments using MAS were performed by the same blinded evaluator, and every effort was made at each site to ensure that the MAS evaluator was the same person throughout the study. Dysport doses were to follow clinical practice for subjects suffering from upper limb spasticity position pattern type 1, 3 or 4 post stroke or traumatic brain injury. The hypothesis for this study was that one low-concentration botulinum neurotoxin type A (BoNT-A) injection per muscle, centrally located in the area/band of the NMJ zones, would spread to and block the surrounding NMJ zones and be as effective as the technique used today in clinical practice. The possibility to reduce the number of injection points would decrease the risk of injection discomfort, pain and injection site bleeding for the patient. A simplified injection technique with one injection per muscle and in a defined location would also benefit physicians. At Baseline (Visit 1), subjects were randomised to one of two treatment groups: - Group 1: Current clinical practice technique and high-concentration dilution: Dysport 300 U/mL. - Group 2: NMJ targeted technique and low-concentration dilution: Dysport 100 U/mL. Each subject visited the clinic on at least three occasions: - Baseline (Visit 1): Screening, randomisation and Dysport treatment. - Week 4 (Visit 2): Treatment follow-up, 4 weeks after Dysport treatment. - Week 12 (Visit 3): Treatment and study follow-up, 12 weeks after Dysport treatment. For subjects not receiving any post study BoNT-A injection at Week 12 due to remaining treatment effect, an extra visit (Visit 4) for study follow-up was to take place at the next routine visit planned for a new BoNT-A injection, at the latest 24 weeks post study injection. The duration of each subject's study period was at a minimum 12 weeks and maximum 24 weeks. The overall duration of the study was planned to be approximately 36 months. ;


Study Design


Related Conditions & MeSH terms


NCT number NCT01682148
Study type Interventional
Source Ipsen
Contact
Status Terminated
Phase Phase 3
Start date September 2012
Completion date March 2015