Clinico‐Genetic, Imaging and Molecular Delineation of COQ8A ‐Ataxia: A Multicenter Study of 59 Patients

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Traschütz, Andreas | Schirinzi, Tommaso | Laugwitz, Lucia | Murray, Nathan | Bingman, Craig | Reich, Selina | Kern, Jan | Heinzmann, Anna | Vasco, Gessica | Bertini, Enrico | Zanni, Ginevra | Durr, Alexandra | Magri, Stefania | Taroni, Franco | Malandrini, Alessandro | Baets, Jonathan | de Jonghe, Peter | de Ridder, Willem | Bereau, Matthieu | Demuth, Stephanie | Ganos, Christos | Basak, a Nazli | Hanagasi, Hasmet | Kurul, Semra Hiz | Bender, Benjamin | Schöls, Ludger | Grasshoff, Ute | Klopstock, Thomas | Horvath, Rita | van de Warrenburg, Bart | Burglen, Lydie | Rougeot, Christelle | Ewenczyk, Claire | Koenig, Michel | Santorelli, Filippo | Anheim, Mathieu | Munhoz, Renato | Haack, Tobias | Distelmaier, Felix | Pagliarini, David | Puccio, Hélène | Synofzik, Matthis

Edité par CCSD ; Wiley -

International audience. Objective: To foster trial-readiness of coenzyme Q8A (COQ8A)-ataxia, we map the clinicogenetic, molecular, and neuroimaging spectrum of COQ8A-ataxia in a large worldwide cohort, and provide first progression data, including treatment response to coenzyme Q10 (CoQ10).Methods: Cross-modal analysis of a multicenter cohort of 59 COQ8A patients, including genotype-phenotype correlations, 3D-protein modeling, in vitro mutation analyses, magnetic resonance imaging (MRI) markers, disease progression, and CoQ10 response data.Results: Fifty-nine patients (39 novel) with 44 pathogenic COQ8A variants (18 novel) were identified. Missense variants demonstrated a pleiotropic range of detrimental effects upon protein modeling and in vitro analysis of purified variants. COQ8A-ataxia presented as variable multisystemic, early-onset cerebellar ataxia, with complicating features ranging from epilepsy (32%) and cognitive impairment (49%) to exercise intolerance (25%) and hyperkinetic movement disorders (41%), including dystonia and myoclonus as presenting symptoms. Multisystemic involvement was more prevalent in missense than biallelic loss-of-function variants (82-93% vs 53%; p = 0.029). Cerebellar atrophy was universal on MRI (100%), with cerebral atrophy or dentate and pontine T2 hyperintensities observed in 28%. Cross-sectional (n = 34) and longitudinal (n = 7) assessments consistently indicated mild-to-moderate progression of ataxia (SARA: 0.45/year). CoQ10 treatment led to improvement by clinical report in 14 of 30 patients, and by quantitative longitudinal assessments in 8 of 11 patients (SARA: -0.81/year). Explorative sample size calculations indicate that ≥48 patients per arm may suffice to demonstrate efficacy for interventions that reduce progression by 50%.Interpretation: This study provides a deeper understanding of the disease, and paves the way toward large-scale natural history studies and treatment trials in COQ8A-ataxia. ANN NEUROL 2020;88:251-263.

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