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The p.A382T TARDBP gene mutation in Sardinian patients affected by Parkinson's disease and other degenerative parkinsonisms
Authors:Antonino Cannas  Giuseppe Borghero  Gian Luca Floris  Paolo Solla  Adriano Chiò  Bryan J. Traynor  Andrea Calvo  Gabriella Restagno  Elisa Majounie  Emanuela Costantino  Valeria Piras  Loredana Lavra  Carla Pani  Gianni Orofino  Francesca Di Stefano  Paolo Tacconi  Marcello Mario Mascia  Antonella Muroni  Maria Rita Murru  Stefania Tranquilli  Daniela Corongiu  Marcella Rolesu  Stefania Cuccu  Francesco Marrosu  Maria Giovanna Marrosu
Affiliation:1. Centro per i Disordini del Movimento, Dipartimento di Scienze Cardiovascolari e Neurologiche, Sezione Neurologia, Policlinico Universitario, Università di Cagliari, SS 554 Bivio Sestu, 09042, Monserrato, Cagliari, Italy
2. Dipartimento di Scienze Cardiovascolari e Neurologiche, Policlinico Universitario, Università di Cagliari, Monserrato, Cagliari, Italy
3. Centro Regionale Esperto per la SLA (CRESLA), Dipartimento di Neuroscienze, Università di Torino, Turin, Italy
4. Laboratory of Neurogenetics, National Institute on Aging, NIH, Bethesda, MD, USA
5. Laboratorio di Genetica Molecolare, ASO OIRM-Sant’Anna, Turin, Italy
6. Laboratorio Centro Sclerosi Multipla, Ospedale Binaghi, Università di Cagliari, Monserrato, Cagliari, Italy
Abstract:Based on our previous finding of the p.A382T founder mutation in ALS patients with concomitant parkinsonism in the Sardinian population, we hypothesized that the same variant may underlie Parkinson's disease (PD) and/or other forms of degenerative parkinsonism on this Mediterranean island. We screened a cohort of 611 patients with PD (544 cases) and other forms of degenerative parkinsonism (67 cases) and 604 unrelated controls for the c.1144G > A (p.A382T) missense mutation of the TARDBP gene. The p.A382T mutation was identified in nine patients with parkinsonism. Of these, five (0.9 % of PD patients) presented a typical PD (two with familiar forms), while four patients (6.0 % of all other forms of parkinsonism) presented a peculiar clinical presentation quite different from classical atypical parkinsonism with an overlap of extrapyramidal–pyramidal–cognitive clinical signs. The mutation was found in eight Sardinian controls (1.3 %) consistent with a founder mutation in the island population. Our findings suggest that the clinical presentation of the p.A382T TARDBP gene mutation may include forms of parkinsonism in which the extrapyramidal signs are the crucial core of the disease at onset. These forms can present PSP or CBD-like clinical signs, with bulbar and/or extrabulbar pyramidal signs and cognitive impairment. No evidence of association has been found between TARDBP gene mutation and typical PD.
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