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Abstract Details

Weight Loss and Increase Insulin Sensitivity in Early Stage Machado-Joseph Disease/Spinocerebellar Ataxia Type 3 (MJD/SCA3) Patients
Movement Disorders
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004
Machado-Joseph disease (MJD/SCA3), caused by a CAG repeat expansion (CAGn) at ATXN3 gene, is usually considered a pure neurological disorder. We have recently described low body mass index (BMI) and high peripheral insulin sensitivity in MJD/SCA3 questioning this concept.
Anthropometry, bioimpedance and glicemic curves, as well as SARA and NESSCA scales, were performed in 44 MJD/SCA3 patients [?10y of disease duration (DD)] and 41 healthy controls with similar environmental background. Pre-symptomatic individuals are under recruitment.
Patients and controls did not differ in age and gender proportions. MJD/SCA3 patients had a m卤sd of 35卤10 years of Age at Onset (AO), 5.7卤2 years of DD, and 75卤3 CAGn. The following data (m卤sd) were obtained in cases and in controls: BMI of 24.3卤4.3 and 27.4卤6.5kg/m2 (p=0.011), lean mass of 74.3卤8.5% and 71.9卤8.6% (ns), basal metabolic rate (BMR) of 23.2卤2.6 and 22.4卤2.6cal/kg (ns), fasting glucose (FG) of 89.2卤8.8 and 94.6卤8.2mg/dL (p=0.005) and after an oral glucose tolerance test (GTT, 120min), of 88.3卤28 and 105.6卤32.6mg/dL (p=0.011). BMI was related to CAGn (R=-0.475, p=0.001) and AO (R=0.485, p=0.001), with no relation to SWAL-Qol dysphagia scale (ns). FG was related to CAGn (R=-0.303, p=0.049) and GTT to AO (R=0.470, p=0.002), independently of CAGn, its main determinant.
Weight loss in MJD/SCA3 affects both lean and fat body masses and is detectable since the first years of disease. Nutritional alterations seem to be primarily related to the disease causative mutation (CAGn) and alterations in insulin pathways might act as disease phenotype modifier.
Authors/Disclosures
Jonas A. Saute, MD
PRESENTER
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Thais Monte No disclosure on file
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