Neurofibromatosis Type 1 Clinical Trial
Official title:
A Randomized Placebo-Controlled Study of Lovastatin in Children With Neurofibromatosis Type 1
The specific aim of this study is to determine whether Lovastatin ™ significantly improves
visual spatial learning and/or sustained attention in children with NF1.
Secondary Aims:
To evaluate the effect of Lovastatin ™ on measures of executive function, behavior and
quality of life in children with NF1 and cognitive deficits.
To further evaluate the toxicity and tolerability of Lovastatin ™ in children with NF1 and
cognitive deficits.
Hypotheses
It is hypothesized that Lovastatin ™ will improve the visual spatial memory and/or attention
deficits in children with NF1. This is based on studies demonstrating that Lovastatin ™ has
significantly improved impairments in visual spatial memory and attention in the NF1 murine
model.
It is further expected that Lovastatin ™ will be safe and well tolerated over a 16-week
period.
Study Design
This is a prospective multi-centre randomized, placebo-controlled Phase II study to determine
the efficacy of Lovastatin ™ on visual spatial learning and/or attention abilities of
children with NF1 aged between 8 and less than 16 years. In addition, the effect of
Lovastatin ™ on secondary measures of executive function, visual spatial skills, behavior and
quality of life will be assessed. Participants will be randomized to 16-weeks of treatment
with Lovastatin ™ or a matched placebo. It is plausible and ethical to employ a placebo group
as no standard therapy with established efficacy is being withheld. There is no cross-over in
this study due to a lack of data concerning the length of possible washout effects. The
Lovastatin ™ dose will begin at 20 mg once daily/continuous dosing and escalate over a
two-week period to 40 mg once daily/continuous dosing and continue at this dose for 14 weeks.
Participants will be carefully monitored for side effects. The safety of Lovastatin ™ will be
evaluated using laboratory tests, clinical signs and adverse effects, which will be monitored
at regular intervals over the 16-week period. Primary and secondary outcome measures will be
administered at baseline, 16 weeks post-treatment and at follow-up, 8 weeks after cessation
of treatment to determine any carry-over effects. The safety of Lovastatin ™ will also be
evaluated, with regular monitoring of side-effects during the trial.
Study Population
This is a Phase II study involving children with NF1 (aged between 8 years to 15 years 11
months old at time of enrollment) with evidence of cognitive impairment, defined as having a
score of at least one standard deviation or more below the population mean on a measure of
visual spatial learning and/or attention.
A total of 142 participants with NF1 aged between 8 years and 15 years 11 months will be
enrolled in the study. The age limits were selected on the basis that Lovastatin ™ has been
shown to be safe in children aged between 8 and 17 years old. In addition, one of the primary
outcome measures (attention) only has normative data for up to 15 years 11 months. Therefore,
the maximum age limit for participants at time of enrolment is 15 years 11 months so that
normative data can be used to determine whether participants are impaired. The pediatric NF1
population is an ideal group in which to study the cognitive effects of Lovastatin ™ because
it represents an opportunity for early pharmacological intervention of cognitive deficits.
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