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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT03682978
Other study ID # AIMS2-CT-01
Secondary ID 2018-000942-21
Status Completed
Phase Phase 2
First received
Last updated
Start date September 19, 2019
Est. completion date January 27, 2023

Study information

Verified date February 2023
Source Celso Arango, MD, PhD
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

AIMS-2-CT-01 is a randomized, double-blind, placebo controlled, study to explore the efficacy, safety and tolerability of Arbaclofen administered to children and adolescents (ages 5-17) for the treatment of social adaptive function in participants with ASD. The effects of Arbaclofen on social function in children and adolescents with ASD will be evaluated in a randomized, placebo controlled, parallel-group study of 16 weeks duration. Subjects who meet protocol criteria will be randomly allocated to receive either Arbaclofen or placebo in a 1:1 ratio in the Treatment Period. There will be 7 recruiting sites and randomization will be stratified by site. A sample of 130 patients will be recruited. Blinding will be maintained by utilizing identical tablets containing either Arbaclofen or placebo.


Description:

Autism Spectrum Disorder (ASD) is a clinically and etiologically heterogeneous neurodevelopmental condition affecting approximately 1% of the population. The core symptoms of ASD are deficits in social communication and the presence of repetitive and restricted behaviours and interests, including sensory anomalies. Currently, there are no effective medical treatments for the core symptoms of ASD, and families frequently use costly non evidence based interventions. Developing drugs for ASD has been challenging because of a limited understanding of its underlying pathophysiology(ies), and difficulties modelling it in vitro and in vivo. A recent study from EU-AIMS reported, for the first time in ASD, that differences in E-I balance can be 'shifted' using a GABA acting drug (riluzole), and that abnormalities in functional connectivity can be 'normalised' by targeting E-I, even in adults. This offers promise that drugs targeting specific parts of the GABA pathway may improve symptoms. The aim of the investigator's project is to conduct a double-blind Randomized Control Trial (RCT) focused on GABA/glutamate equilibrium, to assess the efficacy of a drug that targets core and/or comorbid symptoms in ASD. Arbaclofen is a selective GABA-B receptor agonist and augments GABA-ergic activity, inhibits presynaptic release of glutamate, inhibits postsynaptic transmission, and modulates intracellular signalling. Through elevation of GABA-ergic inhibitory activity, Arbaclofen may act to alleviate ASD symptoms with social anxiety and emotional hyperarousal. Hypothesis: Arbaclofen will be superior to placebo in improving social function as measured by the Vineland-3 social domain.


Recruitment information / eligibility

Status Completed
Enrollment 124
Est. completion date January 27, 2023
Est. primary completion date January 27, 2023
Accepts healthy volunteers No
Gender All
Age group 5 Years to 17 Years
Eligibility Inclusion Criteria: 1. Signed Written Informed Consent 1. Participants or their legal representative must have signed and dated an IRB/IEC approved written informed consent form in accordance with regulatory and institutional guidelines. This must be obtained before the performance of any protocol related procedures that are not part of normal participant care. Participants who do not have the capacity to consent will give developmentally appropriate assent. 2. Participants must be willing and able to comply with scheduled visits, treatment schedule, and laboratory testing. 3. The subject's parent/caregiver/LAR must be able to speak and understand the local language where the study is conducted sufficiently to understand the nature of the study and to allow for the completion of all study assessments. The same parent/caregiver/LAR must be capable of providing reliable information about the subject's condition, agree to oversee the administration of study drug, and accompany the subject to all clinic visits. 4. Patient must be able to speak and understand the local language where the study is conducted sufficiently to understand the nature of the study and to allow for the completion of all study assessments. 2. Type of Participant and Target Disease Characteristics 1. Diagnosis of an Autism Spectrum Disorder according to the DSM-5 criteria 2. Complex language as defined in ADOS-2 to qualify for a Module 3 or 4. 3. Current pharmacological treatment regimen affecting behaviour has been stable for at least 6 weeks prior to screening and is expected to be stable during the duration of the study 4. Current psychotherapeutic/psychosocial interventions affecting behaviour stable for 3 months prior to screening and expected to be stable during the duration of the study (standard regular school breaks and/or annual teacher/classroom change do not qualify for intervention change). 5. Subjects with a history of seizure disorder must currently be receiving stable treatment with anticonvulsant medication and must have been seizure free for 6 months prior to screening, or must be seizure free for 3 years prior to screening if not currently on a stable (>3 months) dose of antiepileptics. 3. Age, Residential and Reproductive Status 1. Male or female participants 5 to 17 years of age at the time of providing consent, inclusive. 2. Reside with the parent/carer who is interviewed for the Vineland. 3. Negative pregnancy test for females of childbearing potential (subject has experienced onset of menses) within 24h prior to study treatment starts. 4. Females of childbearing potential who are sexually active must agree to use a highly effective form of contraception (i.e., existing surgical sterilization, complete abstinence, or a combination of two effective forms of contraception, such as, for example, condoms plus hormonal treatment). 5. Male participants with female partners of childbearing potential are eligible to participate if they agree to the following conditions: - Inform any and all partner(s) of their participation in a clinical drug study and the need to comply with contraception instructions as directed by the investigator. - Male participants are required to use a condom for study duration and until end of relevant systemic exposure defined as 7 months after the end of study treatment. - Female partners of males participating in the study to consider use of effective methods of contraception until the end of relevant systemic exposure, defined as 7 months after the end of treatment in the male participant. - Male participants with a pregnant or breastfeeding partner must agree to remain abstinent from penile vaginal intercourse or use a male condom during each episode of penile penetration during the treatment and until 7 months after the end of study treatment. - Refrain from donating sperm for the duration of the study treatment and until 7 months after the end of study treatment. Exclusion Criteria: 1. Medical Conditions a. Subjects with any condition that might interfere with the conduct of the study, confound interpretation of the study results, or endanger their own well-being. This includes, but is not limited to impairment of renal function, evidence or history of malignancy or any significant haematological, endocrine, respiratory, hepatic, cardiovascular or gastrointestinal disease, including any clinically significant abnormalities on ECG. In general, any co-morbid conditions that may interact with study procedures. 2. Prior/Concomitant Therapy 1. Subjects who are currently receiving treatment with racemic baclofen, vigabatrin, tiagabine, or riluzole or other GABA-related medications (e.g. gabapentin or pregabalin). Only occasional benzodiazepine (or derivative drugs) use (PM, i.e. at night) will be allowed. 2. Subjects who are currently receiving pharmacologic treatment affecting behaviour (see concomitant medication section) need to have a stable dose during the 6 weeks prior to the screening visit and for the duration of the study. 3. Participating in programs including non-pharmacologic educational, behavioural, and/or dietary interventions affecting behaviour, participation in these programs must have been continuous during the 3 months prior to screening and participants or their parent/caregiver/LAR may not electively initiate new or modify ongoing interventions for the duration of the study. Typical school vacations are not considered modifications of stable programming. 4. Subjects who have taken another investigational drug within the last 30 days. 3. Physical and Laboratory Test Findings a. Patients with evidence of any significant hematological, endocrine, cardiovascular (including uncorrected symptomatic congenital heart disease), respiratory, renal, hepatic, or gastrointestinal disease, not including mild common pediatric diseases in these areas that are stable (e.g. mild asthma, constipation, etc.), as judged by the investigator. 4. Study Medication Related 1. Subjects who are not able to take oral medications. 2. Subjects who have a history of hypersensitivity to racemic baclofen. 3. Subjects with rare hereditary problems of galactose intolerance, the lactase deficiency or glucose-galactose malabsorption should not take this medicine. 4. Active peptic ulceration as Baclofen stimulates gastric acid secretion. 5. Porphyria. 5. Other Exclusion Criteria 1. Subjects who are currently engaged in illicit drug use or alcohol abuse, according to DSM-5 criteria. 2. Subjects who have previously participated in a clinical trial of Arbaclofen. 3. Women who are breastfeeding.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Arbaclofen
Arbaclofen tablet.
Placebo
Placebo tablet.

Locations

Country Name City State
France Robert Debré Hospital Paris
Spain Hospital Clínic de Barcelona Barcelona
Spain Servicio de Psiquiatría del Niño y del Adolescente, Hospital General Universitario Gregorio Marañón, SERMAS Madrid
Spain University of Salamanca & Complejo asistencial de Zamora Salamanca
United Kingdom University of Glasgow Glasgow
United Kingdom King's College London London
United Kingdom University of Newcastle upon Tyne Newcastle

Sponsors (2)

Lead Sponsor Collaborator
Celso Arango, MD, PhD UMC Utrecht

Countries where clinical trial is conducted

France,  Spain,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Other Explore whether P1 & N170 amplitude & latency as measures of electrophysiology (EEG) are associated with either response to treatment P1 & N170 amplitude & latency are assessed with a face ERP task. Week 0 + Week 16
Other Explore whether Alpha & Theta power (frontal) and Theta connectivity as measures of electrophysiology (EEG) are associated with either response to treatment Alpha & Theta power (frontal) and Theta connectivity are assessed by watching social and non-social videos. Week 0 + Week 16
Other Explore whether induced power at 10Hz & 40Hz as measures of electrophysiology (EEG) are associated with either response to treatment Induced power at 10Hz & 40Hz is assessed with an Auditory Steady State Response task. Week 0 + Week 16
Other Explore whether induced and evoked power at 6Hz & 10Hz as measures of electrophysiology (EEG) are associated with either response to treatment Induced and evoked power at 6Hz & 10Hz are assessed with a Visual Steady State Response task. Week 0 + Week 16
Other Explore whether P1, N1 amplitude and latency of standard stimuli and Mismatch Negativity (MMN) amplitude and latency as measures of electrophysiology (EEG) are associated with either response to treatment P1, N1 amplitude and latency of standard stimuli and Mismatch Negativity (MMN) amplitude and latency are assessed with a Visual Steady State Response task. Week 0 + Week 16
Other Explore whether Alpha & Theta power and connectivity as measures of electrophysiology (EEG) are associated with either response to treatment Alpha & Theta power and connectivity are assessed with a Resting State task. Week 0 + Week 16
Other Explore the relationship between optional blood biomarkers (DNA) and safety, efficacy, and optimal dosing of Arbaclofen as assessed by the measurements specified in the previous outcome measures. Optional blood biomarkers (DNA): The purpose of this repository is to allow future studies of the relationship between variation in DNA sequence with the safety, efficacy, and optimal dosing of Arbaclofen in the treatment of ASD. Week 0 + Week 16
Primary Effect of Arbaclofen vs. placebo on social function Vineland-3 (socialization domain): The Vineland Adaptive Behavior Scales, Third Edition is designed to assess the personal and social functioning of handicapped and non-handicapped persons. It is a gold standard for the assessment of adaptive functioning. The Socialization domain is one of the 4 adaptive domains assessed by the comprehensive interview form. The other 3 adaptive domains are communication, daily living skills and motor skills. The Socialization domain has 3 subdomains: interpersonal relations, play and leisure and coping skills. Week 0 + Week 16
Secondary Effect of Arbaclofen vs. placebo on measures of global function CGI-I: Clinical Global Impression - Improvement Scale is used to determine the patient's improvement in response to treatment. Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Effect of Arbaclofen vs. placebo on measures of global function CGI-S: The Clinical Global Impression - Severity Scale is used to assess the impairment of neurobehavioral function in study subjects. Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Effect of Arbaclofen vs. placebo on other adaptive domains Vineland-3 (other adaptive domains): The Vineland Adaptive Behavior Scales, Third Edition, other adaptive domains: communication, daily living skills and motor skills. Week 0 + Week 16
Secondary Effect of Arbaclofen on measures of social abilities and responsiveness ADOS-2: The Autism Diagnostic Observation Schedule, Version 2, will be used to assess autistic symptomatology.The ADOS-2 is a standardized protocol for the observation of social and communicative behaviour in children, adolescents, and adults who are suspected of having an ASD. Week -3
Secondary Effect of Arbaclofen on measures of social abilities and responsiveness through BOSCC BOSCC: The Brief Observation of Social Communication Change will be used to to sensitively measure change of core autistic symptoms by observation of a semi-structured social interaction between a child and an examiner. Week 0 + Week 16
Secondary Effect of Arbaclofen on measures of social abilities and responsiveness through SRS-2-P SRS-2-P: The Social Responsiveness Scale (parent version) measures the severity of social impairment in ASD. Week 0 + Week 16
Secondary Effect of Arbaclofen on measures of social abilities and responsiveness through SRS-2-T SRS-2-T: The Social Responsiveness Scale (teacher version) measures the severity of social impairment in ASD. Week 0 + Week 16
Secondary Effect of Arbaclofen on measures of problem behaviours ABC-C: This is the community version of the original residential version of the Aberrant Behaviour Checklist. It is designed to objectively identify five behaviour subscales through observation by the primary caregiver: irritability, lethargy, stereotypy, hyperactivity, and inappropriate speech. Week 0 + Week 4 + Week 8 + Week 12 + Week 16
Secondary Effect of Arbaclofen on measures of problem behaviours CBCL: Child Behaviour Checklist is a caregiver report form identifying problem behaviour in children. Week 0 + Week 16
Secondary Effect of Arbaclofen on other measures of core symptoms AIM: The Autism Impact Measure is designed to measure change in the core symptoms of autism. Week 0 + Week 4 + Week 8 + Week 12 + Week 16
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed with the SMURF SMURF: Safety Monitoring Uniform Research Form. Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed with the ESS-CHAD ESS-CHAD: The Epworth Sleepiness Scale for Children and Adolescents will be employed to evaluate sedation. Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed with the C-SSRS C-SSRS: The Columbia Suicide Severity Rating Scale is used to measure suicidality. Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed with a pulse rate measurement Vital signs: pulse Week -3 + Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed with a body temperature measurement Vital signs: body temperature Week -3 + Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed with a blood pressure measurement Vital signs: blood pressure Week -3 + Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed by measuring weight Weight: Weight (in kg) will be assessed with all outer wear and shoes removed. Week -3 + Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed by measuring height Height: Height (in cm) will be assessed with all outer wear and shoes removed. Week -3 + Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed with the Tanner scale Tanner stage Week -3 + Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16 + Week 18
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed with blood tests Blood tests: CBC, serum chemistry, liver enzymes and renal function. Week -3 + Week 16
Secondary Safety and tolerability of Arbaclofen in children and adolescents with ASD as assessed with blood tests Urine tests: basic urinalysis, toxics (amphetamines, benzodiazepines, barbiturates, marijuana/cannabis, cocaine, opioids (narcotics)) and pregnancy. Drug testing: Week -3 + Week 16, Pregnancy testing: Week -3 + Week 0 + Week 4 + Week 8 + Week 12 + Week 16
Secondary To explore the use and feasibility of digital biomarkers To explore the use and feasibility of digital biomarkers as treatment-responsive measures of core and associated symptoms of ASD Week -3 + Week 0 + Week 2 + Week 4 + Week 6 + Week 8 + Week 12 + Week 16
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