1. DNAJC13 mutation screening in patients with Parkinson's disease from South Italy
- Author
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Monica Gagliardi a, Grazia Annesi a, Radha Procopioa b, Maurizio Morelli b, Grazia Iannello a, Giuseppe Bonapace c, Manuela Mancini b, Giuseppe Nicoletti a, Aldo Quattrone a, and d
- Subjects
Male ,0301 basic medicine ,Nonsynonymous substitution ,Parkinson's disease ,DNA Mutational Analysis ,Disease ,Autosomal dominant form ,03 medical and health sciences ,Exon ,0302 clinical medicine ,Humans ,Coding region ,Medicine ,Genetic Predisposition to Disease ,Gene ,Aged ,Genetics ,Lewy body ,DNAJC13 ,business.industry ,Parkinsonism ,Parkinson Disease ,HSP40 Heat-Shock Proteins ,Middle Aged ,medicine.disease ,030104 developmental biology ,Italy ,Neurology ,Mutation ,Female ,Neurology (clinical) ,Geriatrics and Gerontology ,business ,030217 neurology & neurosurgery - Abstract
Background Parkinson's disease (PD) is the second most common neurodegenerative disorder, and the most common neurodegenerative form of parkinsonism. Recently, a pathogenic mutation (p.N855S) in DNAJC13 was linked to autosomal dominant Lewy body PD in a Dutch–German–Russian Mennonite multi-incident kindred, and was found in five additional patients. In this study, we performed a comprehensive screening of the DNAJC13 gene in familial PD and sporadic PD to assess the frequency of known and novel rare nonsynonymous variants. Methods We screened 563 sporadic and 168 familial PD patients and a control series (n = 1000) for the coding region of DNAJC13. Results Our sequencing analysis identified two carriers of the c.2708G > A (p.R903K) variant in exon 24 of DNAJC13. One of these carriers is a familial PD. Conclusion The p. R903K variant was not found in 1000 healthy controls and it is localized in a functional domain of the DNAJC13 protein. Further studies are necessary to evaluate the role of DNAJC13 variants in PD.
- Published
- 2018