TY - JOUR
T1 - Stepped Treatment for Attention-Deficit/Hyperactivity Disorder and Aggressive Behavior
T2 - A Randomized, Controlled Trial of Adjunctive Risperidone, Divalproex Sodium, or Placebo After Stimulant Medication Optimization
AU - Blader, Joseph C.
AU - Pliszka, Steven R.
AU - Kafantaris, Vivian
AU - Foley, Carmel A.
AU - Carlson, Gabrielle A.
AU - Crowell, Judith A.
AU - Bailey, Brigitte Y.
AU - Sauder, Colin
AU - Daviss, W. Burleson
AU - Sinha, Christa
AU - Matthews, Thomas L.
AU - Margulies, David M.
N1 - Funding Information:
This work was supported by grants R01MH080050 from the National Institute of Mental Health (NIMH; Dr. Blader) and RR1059482 (Stony Brook General Clinical Research Center) and RR018535 (Feinstein Institute for Medical Research General Clinical Research Center) from the National Center for Research Resources .
Funding Information:
This work was supported by grants R01MH080050 from the National Institute of Mental Health (NIMH; Dr. Blader) and RR1059482 (Stony Brook General Clinical Research Center) and RR018535 (Feinstein Institute for Medical Research General Clinical Research Center) from the National Center for Research Resources. Funding acquisition: Blader Disclosure: Dr. Blader has received research support from Texas Health and Human Services and Abbott Laboratories (now AbbVie) and consultant's honoraria from Arbor Pharmaceuticals and Supernus Pharmaceuticals. He has been affiliated with Northwell Health (unsalaried). Dr. Pliszka has received research support from Texas Health and Human Services, Ironshore Pharmaceuticals, and Shire (a Takeda company) and has anticipated funding from Otsuka Pharmaceuticals; received consultant's honoraria from Supernus Pharmaceuticals, Sunovion Pharmaceuticals, and Cingulate Therapeutics; and provided compensated expert testimony on behalf of AstraZeneca and NLS Pharma. Dr. Kafantaris has received investigational drug and placebo supplies for investigator-initiated research from Janssen Pharmaceuticals. Dr. Carlson's spouse, Harold E. Carlson, MD, serves on the Data Safety Monitoring Board for Pfizer and Lundbeck. Drs. Foley, Crowell, Bailey, Sauder, Daviss, Matthews, and Margulies and Mrs. Sinha have reported no biomedical financial interests or potential conflicts of interest.
Publisher Copyright:
© 2020 American Academy of Child and Adolescent Psychiatry
PY - 2021/2
Y1 - 2021/2
N2 - Objective: Stimulant medications are the most prevalent first-line pharmacotherapy for attention-deficit/hyperactivity disorder, but children with aggressive behavior often receive multiagent treatment. There is sparse evidence for the benefits of adjunctive medications when stimulant monotherapy provides inadequate benefit for aggressive behavior, yet the adverse effects of common adjuncts are well established. This study compared the efficacy in reducing aggressive behavior of risperidone (RISP), divalproex sodium (DVPX), and placebo (PBO) added to stimulant medication among childrenwhose symptoms persisted after individually optimized stimulant treatment. Method: This trial enrolled 6- to 12-year-old with attention-deficit/hyperactivity disorder, a disruptive disorder, significant aggressive behavior, and prior stimulant treatment. Open, systematically titrated stimulant treatment identified patients with inadequate reductions in aggressive behavior, who were then randomly assigned to receive adjunctive RISP, DVPX, or PBO under double-blinded conditions for 8 weeks. Family-based behavioral treatment was offered throughout the trial. The primary outcome was the parent-completed Retrospective Modified Overt Aggression Scale. Results: Participants included 175 children (mean [SD] age 9.48 [2.04] years, 19% female). Of participants, 151 completed the stimulant optimization phase, with aggression remitting among 96 (63%), and 45 were randomly assigned to adjunctive treatment groups. The adjunctive RISP group showed greater reductions in aggression ratings than the PBO group (least squares means difference [ΔLSM], −2.33; 95% CI, −3.83 to −0.82; effect size [ES], −1.32), as did the DVPX group (ΔLSM, −1.60; 95% CI, −3.18 to −0.03; ES, −0.91). Mean standardized body mass index scores increased more among RISP-treated participants than participants receiving PBO (ΔLSM, 1.54; 95% CI, 0.68 to 2.40; ES, 0.58). Conclusion: High response rate during the trial's open stimulant optimization phase suggests that rigorous titration of stimulant medication and concurrent behavioral therapy may avert the need for additional medications. Among nonremitters, RISP and DVPX were efficacious adjunctive treatments, although RISP was associated with weight gain. Clinical trial registration information: Effectiveness of Combined Medication Treatment for Aggression in Children With Attention Deficit With Hyperactivity Disorder (The SPICY Study); https://www.clinicaltrials.gov; NCT00794625.
AB - Objective: Stimulant medications are the most prevalent first-line pharmacotherapy for attention-deficit/hyperactivity disorder, but children with aggressive behavior often receive multiagent treatment. There is sparse evidence for the benefits of adjunctive medications when stimulant monotherapy provides inadequate benefit for aggressive behavior, yet the adverse effects of common adjuncts are well established. This study compared the efficacy in reducing aggressive behavior of risperidone (RISP), divalproex sodium (DVPX), and placebo (PBO) added to stimulant medication among childrenwhose symptoms persisted after individually optimized stimulant treatment. Method: This trial enrolled 6- to 12-year-old with attention-deficit/hyperactivity disorder, a disruptive disorder, significant aggressive behavior, and prior stimulant treatment. Open, systematically titrated stimulant treatment identified patients with inadequate reductions in aggressive behavior, who were then randomly assigned to receive adjunctive RISP, DVPX, or PBO under double-blinded conditions for 8 weeks. Family-based behavioral treatment was offered throughout the trial. The primary outcome was the parent-completed Retrospective Modified Overt Aggression Scale. Results: Participants included 175 children (mean [SD] age 9.48 [2.04] years, 19% female). Of participants, 151 completed the stimulant optimization phase, with aggression remitting among 96 (63%), and 45 were randomly assigned to adjunctive treatment groups. The adjunctive RISP group showed greater reductions in aggression ratings than the PBO group (least squares means difference [ΔLSM], −2.33; 95% CI, −3.83 to −0.82; effect size [ES], −1.32), as did the DVPX group (ΔLSM, −1.60; 95% CI, −3.18 to −0.03; ES, −0.91). Mean standardized body mass index scores increased more among RISP-treated participants than participants receiving PBO (ΔLSM, 1.54; 95% CI, 0.68 to 2.40; ES, 0.58). Conclusion: High response rate during the trial's open stimulant optimization phase suggests that rigorous titration of stimulant medication and concurrent behavioral therapy may avert the need for additional medications. Among nonremitters, RISP and DVPX were efficacious adjunctive treatments, although RISP was associated with weight gain. Clinical trial registration information: Effectiveness of Combined Medication Treatment for Aggression in Children With Attention Deficit With Hyperactivity Disorder (The SPICY Study); https://www.clinicaltrials.gov; NCT00794625.
KW - aggression
KW - anticonvulsants
KW - antipsychotic agents
KW - attention deficit and disruptive behavior disorders
KW - central nervous system stimulants
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U2 - 10.1016/j.jaac.2019.12.009
DO - 10.1016/j.jaac.2019.12.009
M3 - Article
C2 - 32007604
AN - SCOPUS:85099506419
SN - 0890-8567
VL - 60
SP - 236
EP - 251
JO - Journal of the American Academy of Child Psychiatry
JF - Journal of the American Academy of Child Psychiatry
IS - 2
ER -