This clinical trial investigates the effects of nicotinamide riboside (vitamin B3) on the disease course of patients with ataxia telangiectasia. Patients will be treated during four consecutive months with nicotinamide riboside (25mg/kg/day), followed by a washout period of two months. Main study parameters/endpoints: Ataxia, dysarthria, quality of life, laboratory parameters.
Rationale: Ataxia Telangiectasia (A-T) is an autosomal recessively inherited neurodegenerative disorder, with a high cancer risk, that also affects the immune and respiratory system. Therapy for A-T is restricted to symptomatic treatment including rehabilitation care, combined with infection prevention and treatment, and screening for pulmonary dysfunction and malignancies. A-T is caused by mutations in the ATM gene. The ATM protein plays a pivotal role in more than 100 different biochemical processes, among which cellular energy metabolism, cell signaling, and DNA repair. Nicotinamide adenine dinucleotide (NAD+) is an essential molecule in many of these processes and studies have shown that NAD+ deficiency plays a role in disease mechanisms underlying DNA repair disorders such as A-T. NAD+ is available in food, but can also be synthesized in the body from its precursors nicotinamide, nicotinic acid, and nicotinamide riboside (NR), as a group called "vitamin B3". Treatment of experimental A-T animal models with NR showed beneficial effects. The aim of this study is to investigate whether treatment with NR during a period of six months may have positive effects on the disease course of patients with A-T. Objective: To investigate the effects of NR on the disease course of patients with ataxia telangiectasia. Study design: Single center, interventional, explorative, open-label proof of concept study. Study population: Patients with A-T (age \>2 years). Intervention (if applicable): Patients will be treated with nicotinamide riboside (25mg/kg/day), during four consecutive months, followed by a washout period of two months. Main study parameters/endpoints: Ataxia, dysarthria, quality of life, laboratory parameters.
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
TREATMENT
Masking
NONE
Enrollment
24
capsules with niagen
Radboudumc
Nijmegen, Netherlands
Ataxia, SARA (Scale of the assesment and rating of ataxia)
Changes in the total score will be measured.
Time frame: change from baseline -1 month - 4 months - 6 months
Ataxia, ICARS (International Cooperative Ataxia Rating Scale)
Changes in the total score will be measured.
Time frame: change from baseline -1 month - 4 months - 6 months
Ataxia, 9-hole pegboard test.
Changes in fastes time of the 9-hole pegboard test will be measured.
Time frame: change from baseline -1 month - 4 months - 6 months
Dysarthria, Radboud dysarthria assesment (RDA)
Changes in maximum performance tasks and severity of dysarthria will be measured.
Time frame: change from baseline -1 month - 4 months - 6 months
Quality of life questionnaire EuroQoL 5 Dimensions 5 Levels (EQ-5D-5L)
Changes in the total quality of life score will be measured.
Time frame: change from baseline -1 month - 4 months - 6 months
Laboratory measurements
Results will be summarized descriptively, with abnormal and clinically notable values/findings being identified
Time frame: change from baseline -1 month - 4 months - 6 months
Intelligibility, Intelligibility in Context Scale (ICS)
Changes in the total score of the Intelligibility in Context Scale (ICS), will be measured.
Time frame: change from baseline -1 month - 4 months - 6 months
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Fatigue, Visual Analogous Scale (VAS)
Changes in the total VAS score will be measured.
Time frame: change from baseline -1 month - 4 months - 6 months