Risperidone in the Treatment of Disruptive Behavioral Symptoms in Children With Autistic and Other Pervasive Developmental Disorders

Shea, Sarah; Turgay, Atilla; Carroll, Alan M.; Schulz, Miklos; Orlik, Herbert; Smith, Isabel M.; Dunbar, Fiona

doi:10.1542/peds.2003-0264-f

Cited by 484 publications

(307 citation statements)

References 18 publications

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“…[5][6][7]29 These positive effects were maintained at least during 1 year, which was the maximum period evaluated in this study. As expected from earlier trials, we found a marked increase in BMI, waist circumference and prolactin levels.…”

Section: Pharmacogenetics Of Risperidone In Autismmentioning

confidence: 68%

“…1 According to a recent survey, 31% of children with autism spectrum disorders take an antipsychotic medication, 2 with risperidone one of the most popular atypical antipsychotics prescribed. Several open trials of risperidone in autism (reviewed in 3,4 ) and three placebo double-blind randomized controlled trials, [5][6][7] reported significant improvements in at least half of the patients evaluated. 4,8 Risperidone was shown to be well tolerated and effective in treating aggressiveness, hyperactivity, irritability, self-injurious behaviours, stereotipies, social withdrawal and lack of interest.…”

Section: Introductionmentioning

confidence: 99%

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Pharmacogenetics of risperidone therapy in autism: association analysis of eight candidate genes with drug efficacy and adverse drug reactions

Almeida²,

et al. 2009

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Little has been reported on the factors, genetic or other, that underlie the variability in individual response, particularly for autism. In this study we simultaneously explored the effects of multiple candidate genes on clinical improvement and occurrence of adverse drug reactions, in 45 autistic patients who received monotherapy with risperidone up to 1 year. Candidate genes involved in the pharmacokinetics (CYP2D6 and ABCB1) and pharmacodynamics (HTR2A, HTR2C, DRD2, DRD3, HTR6) of the drug, and the brain-derived neurotrophic factor (BDNF) gene, were analysed. Using the generalized estimating equation method these genes were tested for association with drug efficacy, assessed with the Autism Treatment Evaluation Checklist, and with safety and tolerability measures, such as prolactin levels, body mass index (BMI), waist circumference and neurological adverse effects, including extrapyramidal movements. Our results confirm that risperidone therapy was very effective in reducing some autism symptoms and caused few serious adverse effects. After adjusting for confounding factors, the HTR2A c.-1438G4A, DRD3 Ser9Gly, HTR2C c.995G4A and ABCB1 1236C4T polymorphisms were predictors for clinical improvement with risperidone therapy. The HTR2A c.-1438G4A, HTR2C c.68G4C (p.C33S), HTR6 c.7154-2542C4T and BDNF c.196G4A (p.V66M) polymorphisms influenced prolactin elevation. HTR2C c.68G4C and CYP2D6 polymorphisms were associated with risperidone-induced increase in BMI or waist circumference. We thus identified for the first time several genes implicated in risperidone efficacy and safety in autism patients. Although association results require replication, given the small sample size, the study makes a preliminary contribution to the personalized therapy of risperidone in autism.

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Section: Pharmacogenetics Of Risperidone In Autismmentioning

confidence: 68%

Section: Introductionmentioning

confidence: 99%

Pharmacogenetics of risperidone therapy in autism: association analysis of eight candidate genes with drug efficacy and adverse drug reactions

Almeida²,

et al. 2009

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“…Maladaptive behaviors are behaviors that interfere with everyday activities, and include self-injurious behavior, withdrawal, uncooperative behavior, aggression, and destruction of property. Although maladaptive behaviors are often exhibited by people with ASD (Aman, Lam, & CollierCrespin, 2003;Hollander, Phillips, & Yeh, 2003;Shea et al, 2004) and are noted as an associated condition in the DSM-IV definition of autism (APA, 2000), there has been relatively little research documenting their prevalence and course. A longitudinal study of 967 children with different types of intellectual disabilities reported that children with autism had higher levels of maladaptive behaviors than children with fragile × syndrome, Williams syndrome, Prader-Willi syndrome, Down syndrome, or children with an intellectual disability with no specified etiology (Tonge & Einfeld, 2003).…”

Section: Prevalence and Change In Maladaptive Behaviors In Adolescencmentioning

confidence: 99%

Change in Autism Symptoms and Maladaptive Behaviors in Adolescents and Adults with an Autism Spectrum Disorder

Shattuck

Seltzer

Greenberg

et al. 2006

J Autism Dev Disord

479

374

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This study examined change prospectively in autism symptoms and maladaptive behaviors during a 4.5 year period in 241 adolescents and adults with an autism spectrum disorder who were 10-52 years old (mean = 22.0) when the study began. Although many individuals' symptoms remained stable, a greater proportion of the sample experienced declines than increases in their level of autism symptoms and maladaptive behaviors, and there were significant improvements in mean levels of symptoms. Individuals with mental retardation had more autism symptoms and maladaptive behaviors than those without mental retardation, and they improved less over time. Compared to adolescents, older sample members (31 and older) had fewer maladaptive behaviors and experienced more improvement in these behaviors over time.

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“…The approval was largely based on the findings from two randomized, controlled trials in 79 and 101 children with autistic disorder and severe behavioral problems. 4,5 In the larger study, children in the risperidone group had a 57% reduction in irritability compared to only a 14% reduction among children in the placebo group (p Ͻ 0.001). 4 A second atypical antipsychotic, aripiprazole, was approved in late 2009 for the same indication (irritability) in children with ASD, based on the results from two 8-week randomized, placebo-controlled trials in 98 and 218 patients.…”

Section: Introductionmentioning

confidence: 91%

Improving the Prediction of Response to Therapy in Autism

Bent

Hendren

2010

Neurotherapeutics

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Summary: Autism is a heterogeneous disorder involving complex mechanisms and systems occurring at diverse times. Because an individual child with autism may have only a subset of all possible abnormalities at a specific time, it may be challenging to identify beneficial effects of an intervention in double-blind, randomized, controlled trials, which compare the mean responses to treatments. Beneficial effects in a small subset of children may be obscured by the lack of effect in the majority. We review the evidence for several potential model systems of biochemical abnormalities that may contribute to the etiology of autism, we describe potential biomarkers or treatment targets for each of these abnormalities, and we provide illustrative treatment trials using this methodology. Potential model systems include immune over and under reactivity, inflammation, oxidative stress, free fatty acid metabolism, mitochondrial dysfunction, and excitotoxicity. Including potential biomarkers and targeted treatments in clinical trials for autism provides a potential method for limiting the heterogeneity of enrolled subjects, which may improve the power of studies to identify beneficial effects of treatments while also improving the understanding of the disease.

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Risperidone in the Treatment of Disruptive Behavioral Symptoms in Children With Autistic and Other Pervasive Developmental Disorders

Cited by 484 publications

References 18 publications

Pharmacogenetics of risperidone therapy in autism: association analysis of eight candidate genes with drug efficacy and adverse drug reactions

Pharmacogenetics of risperidone therapy in autism: association analysis of eight candidate genes with drug efficacy and adverse drug reactions

Change in Autism Symptoms and Maladaptive Behaviors in Adolescents and Adults with an Autism Spectrum Disorder

Improving the Prediction of Response to Therapy in Autism

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