Fragile X Syndrome Clinical Trial
Official title:
Probiotic Intervention for Microbiome Modifications and Consequential Clinical Improvements in Children With Fragile X Syndrome: Pilot Study
The primary objective of this clinical trial is to evaluate efficacy of probiotic mixture which contains Lactobacillus casei, Lactobacillus salivarius and Bifidobacterium breve, in children with Fragile X aged 3-18 years. Specifically, links between microbiome modifications by probiotic mixture and behavioral manifestations and brain processing (eye tracker, EEG analysis) will be assessed. Exploratory objects of this trial are analyses of microbiome composition and assessment of its alterations and modifications (by probiotic mixture) that may lead to clinical improvement and prediction which patients with FXS may be likely to benefit from probiotics treatment. This is open label trial without masking, where each participant receives probiotic for 3 months (12 weeks). It will be single group assignment. The study plans to enroll 15 participants with FXS, aged 3-18 years, both sexes, during 1-year period and complete all study-related activities by January 2025. During the 3-month study period, subjects will attend three visits (screening/baseline, 6-week, and 3-month visits) to the Fragile X Clinic at the Special Hospital for Cerebral Palsy and Developmental Neurology, Belgrade, Serbia. The primary outcome measureswill be Vineland Adaptive Behavior Scales-Third Edition (VABS-III) and eye tracking measures (social gaze and pupillometry). Exploratory endpoint will be microbiome analyses. Secondary outcome measures will be: CGI-S and CGI-I scores, ABC-CFX score, quality of life, sleep habits and EEG analyses.
Status | Recruiting |
Enrollment | 15 |
Est. completion date | December 31, 2024 |
Est. primary completion date | December 31, 2024 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 3 Years to 18 Years |
Eligibility | Inclusion Criteria: 1. Subject has Fragile X syndrome with a molecular genetic confirmation of the full FMR1 mutation or mosaicism. 2. Subject is a male or female age 3 to 18 years. 3. Subject must have a parent or caretaker who is willing to participate in the whole study. 4. Subject and caregiver are able to attend the clinic regularly and reliably. 5. Subject and/or subject's parent/legal authorized representative is able to understand, read, write and speak Serbian fluently to complete study-related materials. 6. Behavioral and other non-pharmacological treatments/interventions must be stable for 4 weeks before screening and must remain stable during the period between screening and the commencement of study probiotic, and throughout the study. Minor changes in hours or times of therapy that are not considered clinically significant will not be exclusionary. Changes in therapies provided through a school program, due to school vacations, are allowed. 7. The use of concomitant medications must be stable, in terms of dose and dosing regimen, for at least 4 weeks prior to Screening and must remain stable during the period between Screening and the commencement of the study; every effort should be made to maintain stable regimens of allowed concomitant medications from the time of commencement of double-blind study medication until the last study assessment. 8. Patient's parent(s), legal authorized guardian(s), or consistent caregiver(s) can understand and sign an informed consent form to participate in the study. For subjects who are not their own legal guardian, subject's parent/legal authorized representative is able to understand and sign an informed consent to participate in the study. 9. Subject and/or subject's parent/legal authorized representative is able to understand, read, write, and speak Serbian fluently to complete study-related materials. Exclusion Criteria: 1. Families that are not cooperative and will not follow through with the demands of this study; 2. Antibiotic use in the last two months (not counting topical antibiotics); 3. Currently taking antibiotics; 4. Any changes in medications, nutritional supplements, therapies, in the last two months, or any plans to change them during the first 3 months of probiotic treatment; 5. Diagnosis of severe gastrointestinal diseases, such as Crohn's Disease, or Ulcerative Colitis; 6. Subject has a life-threatening medical problem or other major systemic illness that compromises health or safety and/or would interfere with this study; 7. Age younger than 3 or older than 18 years. |
Country | Name | City | State |
---|---|---|---|
Serbia | Special Hospital for Cerebral Palsy and Developmental Neurology | Belgrade |
Lead Sponsor | Collaborator |
---|---|
Specila hospital for cerebral palsy and developmental neurology | FRAXA Research Foundation |
Serbia,
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* Note: There are 32 references in all — Click here to view all references
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Other | Microbiome analyses | Microbiome modification (increased diversity of gut microbiota and changes in gut microbiota composition in the direction of beneficial bacteria) before and after probiotics' treatment will be assessed and linked with potential behavioral changes and changes in brain processing in children with FXS. Briefly, DNA extraction will be performed by using the AllPrep Power Fecal DNA/RNA kit (Qiagen, Hilden, Germany), according to the manufacturer's instructions. Profiling of bacteria will be performed by 16S rRNA gene sequencing, using primers targeting V3-V4 region, as recommended by Angebault et al, 2020 [40].
Library preparation will include a single PCR step following a dual barcoding approach. Amplicons library will be sequenced using a MiSeq Reagent Kit v3 (600-cycle) on a Miseq plattform (Illumina). The generated raw outputs (in fastq format) will be analyzed with dada2 R package [41]. |
3 month | |
Primary | 1. Vineland Adaptive Behavior Scales-Third Edition (VABS-III) | The Vineland, which is a gold standard test for assessing adaptive behavior that is widely used in clinical trials, will be administered to the parent/caregiver at baseline and end of treatment/week 12. Subtests include Communication, Daily Living Skills, Socialization, Motor Skills, and Adaptive Behavior Composite. The Vineland has been normed for individuals with intellectual disability and ASD. The third edition includes updated item content to streamline similar items and reduce redundancy, to reflect changes in daily living (e.g., technology) and in conceptions of developmental disabilities (e.g., ASD), and to allow for potential cultural differences by using more generalized wording of certain items | 3 month | |
Primary | Eye tracking | Eye Tracking Measures: Social Gaze and Pupillometry - For individuals with FXS, findings demonstrated that the social gaze measure shows decreased visual fixations on the eye region while viewing human faces (with greater fixation to the nose region), and these individuals show abnormal pupillary dilation, an indication of sympathetic nervous system reactivity, compared with controls [31].
During the experiment, individuals with FXS will sit in front of the monitor at the distance of 65 cm, while stimuli consist of human faces in natural size with different emotional expressions will be presented. This eyetracking system has several benefits that make it conducive to testing individuals with developmentaldisorders, including 35 cm x 30 cm of tolerance to head-motion at 65 cm distance without requiring any head apparatus or restraints. |
3 month | |
Secondary | Clinical Global Impression Scales of Severity (CGI-S) and Improvement (CGI-I) - | These scales are standard assessment for medication studies because it allows the clinician to utilize the history from the parent or caretaker and incorporate it into a clinical rating for the clinical follow up of the patient through the treatment trial. In the initial evaluation of the patient, we will use the CGI-S (severity) to judge the severity of the symptoms with a scale of normal, not at all ill; borderline ill; mildly ill; moderately ill; markedly ill; severely ill; or among the most extremely ill. The CGI-S scale will be utilized at the baseline, the week 6, and end of treatment/week 12 follow-up visits The CGI-I scale will be utilized at the week 6 and end of treatment/week 12 follow-up visits. We will use CGI-I to look at improvement or worsening of symptoms with a scale of very much improved; much improved; minimal improvement; no improvement; minimally worse; or very much worse | 3 month | |
Secondary | The Aberrant Behavior Checklist - Community Edition (ABC-C), scored using the FXS-specific factoring system (ABC-CFX) | This measure will be completed by the parent/caregiver at baseline, and end of treatment/week 12. This parent/caregiver report measure is the gold standard measure of problem and interfering behaviors in clinical trials in developmental disabilities. The ABC asks responders to rate behaviors from 0 "not a problem at all" to 3 "the problem is severe in degree" across 58 questions. Its use has been validated in a variety of clinical populations, including in ASD and FXS, has been used extensively in clinical trials. It has been subjected to utility analysis in FXS and linked to caregiver stress in families [36, 37]. Scores will be analyzed using the FXS-specific factor structure such that 54 of the items resolve into 6 subscales (irritability, lethargy, social avoidance, stereotypic behavior, hyperactivity, and inappropriate speech). | 3 month | |
Secondary | Pediatric Quality of Life Questionnaire (PedsQL) Parent Proxy | This measure consists of a series of questions relating to a child's quality of life and is administered to the caregiver of the child. The parent proxy module designed for children 8-12 years of age will be administered to the caregivers of all subjects, regardless of age, because the questions therein are most appropriate for the overall study population's cognitive age and ability. It will be completed at baseline, week 6, and end of treatment/week 12. For any subjects not in school, questions pertaining to "school" will be replaced with references to "work" or other activities in their life | 3 month | |
Secondary | Child Sleep Habits Questionnaire (CSHQ) | This measure consists of a series of questions relating to the sleep habits of children. It will be completed by caregivers of all subjects, regardless of age, at baseline, and end of treatment/week 12. | 3 month | |
Secondary | EEG analyses | One outcome measure involves examining EEG differences observed in individuals with FXS, such as amplified N1 ERP amplitudes, heightened resting gamma power, and decreased gamma phase-locking in sensory cortices. These EEG abnormalities are believed to signify cortical hyperexcitability resulting from an imbalance between excitatory (glutamate) and inhibitory (GABAergic) mechanisms in FXS, which has been the focus of numerous pharmaceutical remediation studies. We are analyze power in alpha and delta band. | 3 month |
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