Mechanistic Investigation of Therapies for Down Syndrome Regression Disorder
Overview
- Phase
- Phase 2
- Intervention
- Lorazepam
- Conditions
- Down Syndrome
- Sponsor
- University of Colorado, Denver
- Enrollment
- 66
- Locations
- 2
- Primary Endpoint
- Comparison of number and severity of all adverse events.
- Status
- Recruiting
- Last Updated
- last year
Overview
Brief Summary
Individuals with Down syndrome (DS) have an increased risk of numerous co-occurring conditions, including the neuropsychiatric condition known as Down Syndrome Regression Disorder (DSRD). A DSRD diagnosis often includes a sub-acute onset of catatonia, mutism, depersonalization, loss of ability to perform activities of daily living, hallucinations, delusions, and aggression and is most commonly observed in adolescents and young adults.
The study evaluates the safety and efficacy of three currently prescribed therapies: lorazepam, intravenous immunoglobulin (IVIG) and tofacitinib.
Detailed Description
Recent published case reports and clinical experience of the investigators indicate Down Syndrome Regression Disorder (DSRD) may be successfully treated with immune-modulating therapies, in addition to current pharmacologic options. This study is a multidimensional clinical trial designed to advance the understanding of the etiology of DSRD and to evaluate the safety and efficacy of three distinct therapeutic approaches to treating DSRD: (1) the benzodiazepine lorazepam (Ativan™) (2) intravenous immunoglobulin (IVIG, Gammagard™) or (3) the JAK inhibitor tofacitinib (Xeljanz™). Participants will be randomized into one of the three treatment arms above for the 12-week study period, with a subset of participants undergoing an initial 12-week observational period. Specific Aims: 1. To define the relative safety profile of lorazepam, IVIG, and tofacitinib in DSRD. 2. To compare the efficacy of lorazepam, IVIG, and tofacitinib in DSRD. 3. To investigate potential mechanisms underlying DSRD and its response to therapies.
Investigators
Eligibility Criteria
Inclusion Criteria
- •Individuals with DS between the ages of 8 and 30 years, inclusive. DS is broadly defined to include complete trisomy 21, Robertsonian translocation trisomy 21, partial trisomy 21 (segmental duplication), and mosaic trisomy
- •Diagnosis of possible or probable DSRD per 2022 consensus guidelines.
- •Must agree to random treatment assignment.
- •Must agree to complete a washout of any medications intended to treat symptoms of DSRD or that may interfere with study interventions.
- •Must be able to present with a study partner or legal guardian at all study visits.
Exclusion Criteria
- •Weight less than 40 kg.
- •Pregnant or breast feeding.
- •Past or current tobacco smoking.
- •Poor venous access not allowing repeated blood tests or non-compliance with venipuncture requirements.
- •Known allergies, hypersensitivity, or intolerance to lorazepam, IVIG, or tofacitinib.
- •Participants may be excluded for other unforeseen reasons or confounding reasons for DSRD symptoms at the study doctor's discretion.
- •Co-occurring Conditions
- •Any co-occurring genetic disorder.
- •Active symptomatic cardiac disease.
- •Clinically significant chronic or active viral infection, including but not limited to HIV, hepatitis, CMV, EBV, HSV or untreated tuberculosis.
Arms & Interventions
Lorazepam
Participants will receive lorazepam as an oral pill three times daily for 12 weeks as well as titration doses for an additional 4 weeks (approximately).
Intervention: Lorazepam
Intravenous immunoglobulin (IVIG)
Participants will receive 4 doses of IVIG treatment over 12 weeks.
Intervention: Intravenous immunoglobulin (IVIG)
Tofacitinib
Tofacitinib will be administered as an oral pill at 5 mg twice daily over the 12-week study.
Intervention: Tofacitinib
Outcomes
Primary Outcomes
Comparison of number and severity of all adverse events.
Time Frame: Baseline to 14 weeks
A summary of adverse events (AEs) by type and organ system will be reported for the entire study period, along with any statistically significant differences observed in rates of AEs across treatment arms.
Secondary Outcomes
- Change in catatonia by overall score in BFCRS.(Baseline to 12 weeks)
- Time to complete 25-Foot Walk assessment.(Baseline to 12 weeks)
- Total number of errors in visual motor assessment NEPSY-II.(Baseline to 12 weeks)
- Change in expressive language as measured by total number of words used.(Baseline to 12 weeks)
- Change in adaptive skills as measured by the VABS-3 domain level standard score.(Baseline to 12 weeks)
- Change in family impact score as measured by summary score on PedsQL Family Impact Score.(Baseline to 12 weeks)
- Change in quality of life score as measured by PedsQL summary score.(Baseline to 12 weeks)