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Motor outcome measures in patients with <i>FKRP</i> mutations

Amber Gedlinske, Carrie Stephan, Shelley Mockler, Katie M. Laubscher, Karla S. Laubenthal, Cameron D. Crockett, M. Bridget Zimmerman, Katherine D. Mathews

2020Neurology10 citationsDOIOpen Access PDF

Abstract

OBJECTIVE: . METHODS: mutations were evaluated annually with a battery of established motor outcome measures including limited quantitative myometry and timed function measures. Results were analyzed using random coefficient regression to determine annual change in each measure. Due to the nonlinear progression through the lifespan of the study participants, pediatric (<19 years) and adult (≥19 years) cohorts were analyzed separately. Effect of genotype was evaluated in each cohort. RESULTS: Sixty-nine participants (30 pediatric, 44 adult) with at least 2 evaluations were included. There was a small but statistically significant decline in timed motor function measures in both pediatric and adult cohorts. Genotype significantly affected rate of decline in the pediatric but not the adult cohort. Some pediatric patients who are homozygous for the c.826C>A mutation showed improving motor performance in adolescence. Performance on the 10-meter walk/run was highly correlated with other timed function tests. CONCLUSIONS: mutations that can be detected with standard motor outcome measures, while the results in the pediatric population were more variable and affected by genotype. Overall, these analyses provide a framework for development of future clinical trials. The dystroglycanopathies natural history study (Clinical Trial Readiness for the Dystroglycanopathies) may be found on clinicaltrials.gov (NCT00313677).

Topics & Concepts

Outcome (game theory)MedicineInternal medicineOncologyPhysical medicine and rehabilitationMathematicsMathematical economicsMuscle Physiology and DisordersGenetic Neurodegenerative DiseasesSignaling Pathways in Disease
Motor outcome measures in patients with <i>FKRP</i> mutations | Litcius