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Co-occurring WARS2 and CHRNA6 mutations in a child with a severe form of infantile parkinsonism.

Simone Martinelli, Viviana Cordeddu, Serena Galosi, Ambra Lanzo, Eleonora Palma, Luca Pannone, Andrea Ciolfi, Michela Di Nottia, Teresa Rizza, Gianfranco Bocchinfuso, Alice Traversa, Viviana Caputo, Andrea Farrotti, Claudia Carducci, Laura Bernardini, Susanna Cogo, Maria Paglione, Martina Venditti, Annarita Bentivoglio, Joanne Ng, Manju A Kurian, Laura Civiero, Elisa Greggio, Lorenzo Stella, Flavia Trettel, Miriam Sciaccaluga, Cristina Roseti, Rosalba Carrozzo, Sergio Fucile, Cristina Limatola, Elia Di Schiavi, Marco Tartaglia, Vincenzo Leuzzi

Parkinsonism & related disorders 2020 Mar


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    To investigate the molecular cause(s) underlying a severe form of infantile-onset parkinsonism and characterize functionally the identified variants. A trio-based whole exome sequencing (WES) approach was used to identify the candidate variants underlying the disorder. In silico modeling, and in vitro and in vivo studies were performed to explore the impact of these variants on protein function and relevant cellular processes. WES analysis identified biallelic variants in WARS2, encoding the mitochondrial tryptophanyl tRNA synthetase (mtTrpRS), a gene whose mutations have recently been associated with multiple neurological phenotypes, including childhood-onset, levodopa-responsive or unresponsive parkinsonism in a few patients. A substantial reduction of mtTrpRS levels in mitochondria and reduced OXPHOS function was demonstrated, supporting their pathogenicity. Based on the infantile-onset and severity of the phenotype, additional variants were considered as possible genetic modifiers. Functional assessment of a selected panel of candidates pointed to a de novo missense mutation in CHRNA6, encoding the α6 subunit of neuronal nicotinic receptors, which are involved in the cholinergic modulation of dopamine release in the striatum, as a second event likely contributing to the phenotype. In silico, in vitro (Xenopus oocytes and GH4C1 cells) and in vivo (C. elegans) analyses demonstrated the disruptive effects of the mutation on acetylcholine receptor structure and function. Our findings consolidate the association between biallelic WARS2 mutations and movement disorders, and suggest CHRNA6 as a genetic modifier of the phenotype. Copyright © 2020 Elsevier Ltd. All rights reserved.

    Citation

    Simone Martinelli, Viviana Cordeddu, Serena Galosi, Ambra Lanzo, Eleonora Palma, Luca Pannone, Andrea Ciolfi, Michela Di Nottia, Teresa Rizza, Gianfranco Bocchinfuso, Alice Traversa, Viviana Caputo, Andrea Farrotti, Claudia Carducci, Laura Bernardini, Susanna Cogo, Maria Paglione, Martina Venditti, Annarita Bentivoglio, Joanne Ng, Manju A Kurian, Laura Civiero, Elisa Greggio, Lorenzo Stella, Flavia Trettel, Miriam Sciaccaluga, Cristina Roseti, Rosalba Carrozzo, Sergio Fucile, Cristina Limatola, Elia Di Schiavi, Marco Tartaglia, Vincenzo Leuzzi. Co-occurring WARS2 and CHRNA6 mutations in a child with a severe form of infantile parkinsonism. Parkinsonism & related disorders. 2020 Mar;72:75-79

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    PMID: 32120303

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