A Mutation in VPS35, Encoding a Subunit of the Retromer Complex, Causes Late-Onset Parkinson Disease |
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| Authors: | Alexander Zimprich Anna Benet-Pagès Walter Struhal Elisabeth Graf Sebastian H Eck Marc N Offman Dietrich Haubenberger Sabine Spielberger Eva C Schulte Peter Lichtner Shaila C Rossle Norman Klopp Elisabeth Wolf Klaus Seppi Walter Pirker Stefan Presslauer Brit Mollenhauer Regina Katzenschlager Thomas Foki Christoph Hotzy Eva Reinthaler Ashot Harutyunyan Robert Kralovics Annette Peters Fritz Zimprich Thomas Brücke Werner Poewe Eduard Auff Claudia Trenkwalder Burkhard Rost Gerhard Ransmayr Juliane Winkelmann Thomas Meitinger Tim M Strom |
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| Institution: | 1Department of Neurology, Medizinische Universität Wien, 1090 Vienna, Austria;2Institute of Human Genetics, Helmholtz Zentrum München, German Research Center for Environmental Health, 85764 Neuherberg, Germany;3Department of Neurology and Psychiatry, Allgemeines Krankenhaus, 4021 Linz, Austria;4Institute of Bioinformatics, Technische Universität München, 85748 Garching, Germany;5Department of Neurology, Medizinische Universität Innsbruck, 6020 Innsbruck, Austria;6Department of Neurology, Technische Universität München, 81675 Munich, Germany;7Institute of Epidemiology, Helmholtz Zentrum München, German Research Center for Environmental Health, 85764 Neuherberg, Germany;8Department of Neurology, Wilhelminenspital, 1160 Vienna, Austria;9Paracelsus-Elena Klinik, 34128 Kassel, Germany;10Department of Neurology, Sozialmedizinisches Zentrum Ost-Donauspital, 1220Vienna, Austria;11Center for Molecular Medicine of the Austrian Academy of Sciences, 1090 Vienna, Austria;12Department of Clinical Neurophysiology, Georg-August-Universität Göttingen, 37079 Göttingen, Germany;13Institute of Human Genetics, Technische Universität München, 81675 Munich, Germany |
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| Abstract: | To identify rare causal variants in late-onset Parkinson disease (PD), we investigated an Austrian family with 16 affected individuals by exome sequencing. We found a missense mutation, c.1858G>A (p.Asp620Asn), in the VPS35 gene in all seven affected family members who are alive. By screening additional PD cases, we saw the same variant cosegregating with the disease in an autosomal-dominant mode with high but incomplete penetrance in two further families with five and ten affected members, respectively. The mean age of onset in the affected individuals was 53 years. Genotyping showed that the shared haplotype extends across 65 kilobases around VPS35. Screening the entire VPS35 coding sequence in an additional 860 cases and 1014 controls revealed six further nonsynonymous missense variants. Three were only present in cases, two were only present in controls, and one was present in cases and controls. The familial mutation p.Asp620Asn and a further variant, c.1570C>T (p.Arg524Trp), detected in a sporadic PD case were predicted to be damaging by sequence-based and molecular-dynamics analyses. VPS35 is a component of the retromer complex and mediates retrograde transport between endosomes and the trans-Golgi network, and it has recently been found to be involved in Alzheimer disease. |
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