We propose a study on Ataxia with oculomotor apraxia type 1 (AOA1) in which Coenzyme Q10 (CoQ10) deficit has been observed. Main objectives of the study are : * To monitor evolution of albumin in patients affected with AOA1 while supplemented with CoQ10 ; * To measure with clinical scales and biological markers efficacy of supplementation on disease evolution. AOA1 is characterised by Hypoalbuminemia. Disease duration is negatively correlated with albumin level. This study aims to understand mechanisms of the disease and our hypothesis is that correction or stabilization of albumin level with CoQ10 supplementation could impact disease evolution. The study is planned from 1 to 2 years supplementation. The CoQ10 is classified as a food supplement and has already been tested in other neurological conditions.
Ataxia with ocular apraxia type 1 (AOA1) is an autosomal recessive cerebellar ataxia. Patients' phenotype associates early onset cerebellar ataxia, oculomotor apraxia, neuropathy and often intellectual disability, hypoalbuminaemia and hypercholesterolemia. APTX gene mutations responsible for AOA1 disease were identified in a family previously reported with ataxia and Coenzyme Q10 deficiency. Therefore we measured muscle Coenzyme Q10 in six patients AOA1 and found decreased levels in five. Hypercholesterolaemia and low albumin levels represent hallmarks of the disease. We thus propose therapeutic trial with Coenzyme Q10 in AOA1 patients, by using albumin evolution as primary endpoint. Moreover several secondary endpoints will be performed: * clinical examination (SARA scale) * quantitative assessments of the ataxia (with the calculation of the Composite Cerebellar Functional Severity CCFS) * biological criteria (prealbumin, cholesterol, alphafoetoprotein, blood count, hepatic checkup) * oculographic examination. The study is a multicentric randomised placebo controlled trial with two-year follow-up: * during the first year, one group will be supplemented with Coenzyme Q10 while the other group will receive a placebo; * during the second year, all patients will be supplemented with Coenzyme Q10 in order to assess long term safety and tolerance of the treatment.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
QUADRUPLE
Enrollment
19
• 2 dosages according to patient weight: Weight \< 50kg : 20 drops 3 times a day (150 mg / d) Weight ≥ 50 kg : 40 drops 3 times a day (300 mg / d)
• according to patient weight: Weight \< 50kg : 20 drops 3 times a day Weight ≥ 50 kg : 40 drops 3 times a day
ICM Institute
Paris, France
Albuminemia
Evolution of albuminemia every 6 months during 2 years.
Time frame: 2 years
SARA scale
Evolution of clinical criteria (SARA and CCFS, which represent quantitative scales to assess cerebellar ataxia evolution)
Time frame: 2 years
CCFS
Evolution of clinical criteria (SARA and CCFS, which represent quantitative scales to assess cerebellar ataxia evolution)
Time frame: 2 years
prealbuminemia
Evolution of biological criteria (prealbuminemia, cholesterol, alfa-foeto-protein) every 6 months during 2 years.
Time frame: 2 years
cholesterol
Evolution of biological criteria (prealbuminemia, cholesterol, alfa-foeto-protein) every 6 months during 2 years.
Time frame: 2 years.
alfa-foeto-protein
Evolution of biological criteria (prealbuminemia, cholesterol, alfa-foeto-protein) every 6 months during 2 years.
Time frame: 2 years.
Oculomotor evaluation
Oculomotor evaluation to assess oculo motor apraxia evolution \[Time Frame: Each year during 2 years.\]
Time frame: 2 years
EQ5D - PHQ9
Quality of life evolution (self-administered questionnaire EQ5D - PHQ9) every 6 months during 2 years.
Time frame: 2 years
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