Treatments for Fathers With ADHD and Their At-Risk Children (Fathers Too)

Attention Deficit/Hyperactivity Disorder (ADHD) Clinical Trial

Official title:

Treatments for Fathers With Attention Deficit/Hyperactivity Disorder (ADHD) and Their At-Risk Children (Fathers Too)

Clinical Trial Details — Status: Completed

Administrative data

• NCT number: NCT02675400
• Other study ID #: Fathers Too
• Status: Completed
• Phase: Phase 4
• Start date: December 2015
• Est. completion date: August 31, 2018

Study information

• Verified date: September 2018
• Source: Seattle Children's Hospital
• Contact: n/a
• Is FDA regulated: No
• Study type: Interventional

Clinical Trial Summary

In contrast to mothers with Attention Deficit/Hyperactivity Disorder (ADHD), the impact of paternal ADHD in families and children with ADHD symptoms has not been studied, despite the prevalence of ADHD in males. Thus, the investigators do not know the feasibility, impact on treatment on the family and child, and effects of treating fathers relative to mothers with ADHD. Paternal ADHD is associated with negative parenting and child conduct problems.

The investigators hypothesize that successfully treating parental ADHD in fathers will have a beneficial effects on the family that will extend to the child. Specifically, the investigators believe that stimulant medication ((Lisdexamfetamine (LDX) or a different ADHD medication if poor response to LDX) with fathers will reduce father's ADHD symptoms and improve parenting. Effects of stimulant treatment of fathers will be compared to Behavioral Parent Training (BPT) on parenting, and paternal and child outcomes in fathers with ADHD who have children between the ages of 3 -8.

As in the investigator's previous work, the investigators will bank paternal and child DNA and RNA for later examination of pharmacogenetic and epigenetic effects (i.e. RNA) of stimulant response.

Description:

The overarching goal of this research program is to construct and evaluate paternal and familial interventions to improve the trajectory of ADHD outcomes in at-risk young children with ADHD symptoms who have not yet been treated with stimulant medications. These children are at risk for ADHD by virtue of paternal ADHD and maladaptive parenting. Our primary outcome measure for the child will be whether child ADHD symptoms on the Conners Parent and Teacher Rating Scales decreased at the completion of the study. The primary outcomes for the fathers will be the Conners Adult ADHD Rating Scale-Self Report and Other Report (CAARS), the clinician completed Clinical Global Impressions-Severity (CGI-S) and the Barkley Functional Impairment rating Scale (BFIS). Secondary outcomes include the Family Routines Questionnaire (FRI), the Alabama Parent Questionnaire (APQ) and the Dyadic Parent-Child Interaction Coding System (DPICS).

Specific Aim 1: To develop screening and recruitment strategies for identifying fathers with ADHD who have young children at risk for ADHD.

Specific Aim 2: To assess the comparative efficacy of treating fathers with LDX (or a different ADHD medication if poor response to LDX) and functional impairment after 8 weeks of treatment.

Hypothesis 1a: LDX will be associated with a greater reduction in paternal ADHD symptoms (CAARS, CAARS-Other Informant) and impairment (CGI-S) than families treated with BPT.

Hypothesis 1 b: BPT will be associated with greater improvement on measures of parenting (e.g. APQ, DPICS) and family functioning (DAS, BFIS) than LDX.

To the investigator's knowledge, this 2.5 year study will be the very first to examine the benefit of identifying and treating fathers with ADHD prior to treating the at-risk child. In addition, to the investigator's knowledge, this is the first study to directly compare the impact of BPT vs. LDX on both father and child outcomes. Thus, the investigator's propose a novel treatment strategy for a not uncommon but difficult to treat patient population: young children who are at risk for ADHD by virtue of their early-onset behavior problems and environmental factors such a poor parenting.

Recruitment information / eligibility

• Status: Completed
• Enrollment: 19
• Est. completion date: August 31, 2018
• Est. primary completion date: August 31, 2018
• Accepts healthy volunteers: Accepts Healthy Volunteers
• Gender: Male
• Age group: 21 Years to 55 Years

Eligibility

Fathers Inclusion Criteria:

• Sign informed consent

• Be between 21-55 years old (inclusive) at the screening visit

• English-speaking

• At screening (after washout, if required) meet full DSM-IV criteria for ADHD, any subtype

• Current CGI-S-ADHD rating = 4 and < 7.

• Findings on physical exam (PE), laboratory studies, vital signs, and electrocardiogram (ECG) judged to be normal for age with no contraindications for MPH treatment.

• Pulse and blood pressure (BP) within 95% of age and gender mean

• Commit to the entire visit schedule for the study.

• Able to complete all study assessments.

• Fathers with comorbid mood/anxiety disorders which are effectively treated with antidepressants or anti-anxiety agents will be eligible for participation, provided this medication has not changed within 30 days, is well tolerated, and that current mood symptoms are not severe or associated with active suicidal ideation.

Father Exclusion Criteria:

• History of allergic reactions or severe negative response to study medications

• Active alcohol/substance abuse in the past 3 months or a positive urinary toxic screen on initial evaluation that is not explained by a time-limited medical circumstance.

• Current bipolar illness, schizophrenia, psychoses, or significant suicidal risk

• History of chronic or acute medical disorder for which stimulant therapy would be contraindicated (e.g., glaucoma, hypertension).

• Currently, (or within the past 30 days) receiving stimulant medication for ADHD.

• Father should not seek parent-based interventions during the course of the study, Weeks 1 - 8.

Child Inclusion Criteria:

• Sign assent if older than six.

• Be between the ages of 3-8.

• Symptoms of ADHD (Conners Hyperactivity Index or Attention > 60).

• English speaking.

• No prior treatment with effective doses of stimulants.

Related Conditions & MeSH terms

• Attention Deficit Disorder with Hyperactivity
• Attention Deficit/Hyperactivity Disorder (ADHD)
• Hyperkinesis

Intervention

Drug:
• Vyvanse
Half of the participants (fathers) will be randomized to receive Vyvanse.

Behavioral:
• Behavioral Parent Training
Half of the fathers will receive behavioral parent training.

Drug:
• Methylphenidate
If Vyvanse is not well tolerated, methylphenidate can be prescribed.

Locations

Country	Name	City	State
United States	Seattle Children's	Seattle	Washington

Sponsors (1)

Lead Sponsor	Collaborator
Seattle Children's Hospital

Country where clinical trial is conducted

United States, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	CGI -S - ADHD rating scale (Father)	Clinical Global Impression - Severity .	Change from Screening at 8 weeks.
Primary	Conners Adult ADHD Rating Scale - Self Report (Father)	This is a 93-item, reliable and valid measure assessing the core features of DSM-IV ADHD, while adding content unique to the adult expression of ADHD	Change from Screening at 8 weeks.
Primary	Conners Other Report (about Father)	Completed by collateral informant. The Conners Other Report is a reliable and valid measure assessing the core features of DSM-IV ADHD, while adding content unique to the adult expression of ADHD	Change from Screening at 8 weeks
Primary	Barkley Functional Impairment Rating Scale (Father)	The BFIS is a promising measure of impairment associated with adult ADHD, with adequate reliability, criterion validity with other measures of impairment, and normative data for adults. Normative data and reliable change index will allow for assessing functioning in domains relevant to the current proposal (i.e. Home-family, Daily Responsibilities, Child Rearing) as Well as Mean Impairment Score are sensitive to treatment effects.	Change from Screening at 8 weeks.
Primary	Conners Parent (completed by parent about child)	Conners Parent Rating Scale that results in factor scores for Oppositional Behavior, Cognitive Problems, and Hyperactivity. There is extensive normative data and evidence of reliability, validity, and clinical utility (Hart, 1999). This will be the primary measure specifically for ADHD and externalizing symptoms.	Change form Screening at 8 weeks.
Primary	Conners Teacher Rating Scale (completed by teacher about child)	Conners Teacher Rating Scale that results in factor scores for Oppositional Behavior, Cognitive Problems, and Hyperactivity. There is extensive normative data and evidence of reliability, validity, and clinical utility (Hart, 1999). This will be the primary measure specifically for ADHD and externalizing symptoms.	Change from Screening at 8 weeks.
Secondary	Barkley Functional Impairment Rating Scale (BFIS) - Other	Completed by collateral informant. The BFIS is a promising measure of impairment associated with adult ADHD, with adequate reliability, criterion validity with other measures of impairment, and normative data for adults. Normative data and reliable change index will allow for assessing functioning in domains relevant to the current proposal (i.e. Home-family, Daily Responsibilities, Child Rearing) as Well as Mean Impairment Score are sensitive to treatment effects.	Change from Baseline at 8 Weeks.
Secondary	Family Routines Inventory (FRI)	The FRI is a 26-item parent-report measure that assesses the frequency with which families engage in a broad range of routines.	Change from Baseline at 8 Weeks.
Secondary	Alabama Parenting Questionnaire (APQ)	is a 42-item measure on which parents are asked to indicate the frequency with which they implement the following parenting practices: Corporal Punishment, Inconsistent Discipline, Poor Monitoring/Supervision, Involvement, and Positive Parenting.	Change from Baseline at 8 Weeks.
Secondary	Dyadic Parent-Child Interactions (DPICS)	Parents and children will engage in 3 tasks.	Change from Baseline at 8 Weeks.