Autistic Disorder Clinical Trial
Official title:
Placebo-Controlled Study of Risperidone for the Treatment of Children and Adolescents With Autism and Negative Behavioral Symptoms
This study is designed to determine the effectiveness of risperidone, a drug treatment for
the interfering symptoms of Autistic Disorder in children and adolescents between the ages
of 5 and 17. Between 100 and 120 patients will be participating in this research study at
five academic medical centers in the United States. The primary aim of the treatment is to
reduce impairing behavioral symptoms such as aggression, explosive outbursts, or
self-injurious behavior, without significant side effects. A secondary aim is to evaluate
possible improvement in the level of social relatedness, attention, motor coordination, and
short-term memory.
This study is a placebo-controlled, double-blind study (neither the investigators nor
patients know if the treatment being given is risperidone or an inactive substance,
placebo). Patients will be asked to participate for 6 to 8 months. For the first 8 weeks,
patients will receive either risperidone or placebo, randomly chosen. At the end of the 8
weeks, those patients who have improved and were on risperidone will be asked to continue on
this medication for another 4 months. The last two months of the study are again
double-blind (neither patients nor investigators know treatment). Patients will either
continue risperidone treatment or be gradually tapered from risperidone
(placebo-substitution). This blinded discontinuation phase will last 2 months during which
patients will be closely monitored for recurrence or worsening of symptoms. Patients who
have been treated with placebo in the first 8 weeks of the study and have not improved will
be treated with risperidone. Weekly visits are required for the first 8 weeks of the study,
monthly visits for the following 4 months, and weekly visits during the last 2 months of the
study.
The primary purpose of this study is to compare the relative safety and efficacy of
risperidone and placebo in the treatment of children and adolescents with autistic disorder.
HYPOTHESES: (1) Risperidone will be more effective than placebo in reducing impulsive
aggression, agitation, self-injurious behavior, and troublesome repetitive behavior
associated with autism. (2) Risperidone will result in more sedation (transient) and weight
gain than placebo. (3) Patients continued on risperidone will be significantly less likely
to experience exacerbation of symptoms of irritability, aggression, agitation, and
stereotypy than those randomized to placebo, as measured by the Aberrant Behavior Checklist
(ABC), the Ritvo-Freeman Real Life Rating Scale, and the compulsions scale from the
Children's Yale-Brown Obsessive Compulsive Scale (CY-BOCS). (4) Patients continued on
risperidone would show superior adjustment and functioning at the end of the trial, as
evidenced by lower Clinical Global Impression ratings, when compared to patients randomized
to placebo.
Design Phase I: Double-Blind Phase - Randomized, double-blind, placebo-controlled, parallel
groups design. Eight-week double-blind treatment with risperidone or placebo. Eight-week
open trial with risperidone for placebo non-responders (patients who were randomized to
placebo and showed no improvement).
(Risperidone responders will be eligible to enter the four-month extension study. Placebo
responders and risperidone non-responders will be managed as clinically appropriate by each
research site.) Phase II: Extension Study - Four-month, open treatment with risperidone.
Dose adjustment permitted according to clinical assessment (efficacy or adverse events).
Two-month, randomized, double-blind, placebo-controlled discontinuation, parallel group
design.
Completers of four-month Extension Phase protocol who have maintained significantly improved
status (decrease greater than 25% in ABC from Protocol I Baseline ratings and CGI of much or
very much improved) will be randomized at the end of four months to placebo substitution or
risperidone continuation. Group assigned to placebo substitution will undergo weekly blinded
reductions of entry dose (dosage at end of Phase I) by 25% per week over three consecutive
weeks. After full placebo substitution, placebo group will remain on placebo for total of up
to 5 weeks (three-week taper, five-week remaining on placebo). Group assigned to continued
active treatment will be maintained on entry dose level for full 8 weeks of Phase II,
assuming no behavioral deterioration. Active treatment patients may have dose reduced for
treatment emergent effects.
Randomization - Balanced within site by Tanner Stage (pre-pubertal: Tanner I or II as
measured by the absence of pubic hair; post-pubertal: Tanner III or greater), gender, and
anticonvulsant use.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Masking: Double-Blind, Primary Purpose: Treatment
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