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. 2019 Oct 8;2019(10):CD001408. doi: 10.1002/14651858.CD001408.pub2

Baker 2002.

Methods Method of randomisation: computer‐generated sequence with block randomisation, stratified by centre and baseline spasticity component
Blinding: all participants and personnel blinded to the intervention
Intention‐to‐treat analysis: yes
Loss of follow‐up: 2

  • BoNT‐A 30 U/kg group: 1 withdrew before treatment

  • BoNT‐A 20 U/kg group: 1 lost to follow‐up in week 8


Unit of analysis: lower limb for local measures and child for global measures
Participants Place: 6 centres in the UK, 1 in Ireland, and 5 in Poland
Period of study: not described
Number assigned: 126
Number assessed: 124

  • 29 BoNT‐A 30 U/kg group

  • 27 BoNT‐A 20 U/kg group

  • 36 BoNT‐A 10 U/kg group

  • 31 placebo group


Inclusion criteria:

  • Spastic diplegic CP

  • Aged 2 to 9 years

  • Weight 10 to 25 kg

  • Ambulatory with or without walking aids

  • Dynamic component

  • Indication of BoNT‐A treatment


Exclusion criteria:

  • Previous BoNT‐A treatment within 9 months

  • Previous phenol treatment

  • Previous muscle or ligament surgery in the lower limbs


Age:

  • BoNT‐A 20 U/kg group (mean (SD)): 4.9 (1.9)

  • Placebo group (mean (SD)): 5.5 (2.2)


Gender:

  • BoNT‐A 20 U/kg group: 46% males; 54% females

  • Placebo group: 55% males; 45% females


Motor distribution:

  • Only spastic diplegia


GMFCS:

  • BoNT‐A group: 11 level I; 1 level II

  • Placebo group: 14 level l; 0 level II
Interventions BoNT‐A groups:

  • Single BoNT‐A (abobotulinumtoxinA) injection into the gastrocnemius in 3 different doses (10, 20, and 30 U/kg)

  • Oral antispasticity medication, regular physiotherapy, walking aids and/or orthoses were all maintained in the course of the study


Placebo group:

  • Single placebo injections into the gastrocnemius

  • Oral antispasticity medication, regular physiotherapy, walking aids and/or orthoses were all maintained in the course of the study
Outcomes Length of follow‐up:

  • Follow‐up of 16 weeks

  • Assessments at baseline, 4, 8, and 16 weeks


Primary outcomes:

  • Change in the dynamic component of gastrocnemius shortening at 4 weeks (assessed by flexible electrogoniometers)

  • Adverse events


Secondary outcomes:

  • Ankle range of motion

  • Gross Motor Function Measure
Notes Comments:

  1. This was a dose‐range study. For the purposes of this review, we analysed the main outcomes only for the intermediate‐dose group (20 U/kg) versus placebo. For the analysis of adverse events, we pooled data from all the BoNT‐A groups in the study.


Source of funding: Ipsen Limited
Conflicts of interest: not reported, but the grant mentioned above could be considered as a possible conflict of interest.
Risk of bias
Bias Authors' judgement Support for judgement
Random sequence generation (selection bias) Low risk Comment: computer‐generated sequence
Allocation concealment (selection bias) Low risk Comment: allocation concealed
Blinding of participants and personnel (performance bias) 
 All outcomes Low risk Comment: blinding of participants and personnel
Blinding of outcome assessment (detection bias) 
 All outcomes Low risk Comment: group assignments were not released until the final assessment and completion of data analysis
Incomplete outcome data (attrition bias) 
 All outcomes Low risk Comment: no missing outcome data
Selective reporting (reporting bias) Unclear risk Comment: study protocol not available. The relevant outcomes seem to have been reported.
Other bias Low risk Comment: no other sources of bias identified