ATP13A2 variants in early-onset Parkinson's disease patients and controls

Djarmati, Ana; Hagenah, Johann; Reetz, Kathrin; Winkler, Susen; Behrens Pellegrino, María Isabel; Pawlack, Heike; Lohmann, Katja; Ramirez, Alfredo; Tadić, Vera; Brüggemann, Norbert; Berg, Daniela; Siebner, Hartwig R.; Lang, Anthony E.; Pramstaller, Peter P.; Binkofski, Ferdinand

Artículo de revista

Fecha

2009

Registro en:

Movement Disorders, Volumen 24, Issue 14, 2018, Pages 2104-2111

15318257

08853185

10.1002/mds.22728

https://repositorio.uchile.cl/handle/2250/164891

Autor

Djarmati, Ana

Hagenah, Johann

Reetz, Kathrin

Winkler, Susen

Behrens Pellegrino, María Isabel

Pawlack, Heike

Lohmann, Katja

Ramirez, Alfredo

Tadić, Vera

Brüggemann, Norbert

Berg, Daniela

Siebner, Hartwig R.

Lang, Anthony E.

Pramstaller, Peter P.

Binkofski, Ferdinand

Institución

Universidad de Chile

Resumen

Four genes responsible for recessively inherited forms of Parkinson's disease (PD) have been identified, including the recently discovered ATP13A2 (PARK9) gene. Our objective was to investigate the role of this gene in a large cohort of PD patients and controls. We extensively screened all 29 exons of the ATP13A2 coding region in 112 patients with early-onset PD (EOPD; <40 years) of mostly European ethnic origin and of 55 controls. We identified four carriers (3.6%) of novel single heterozygous ATP13A2 missense changes that were absent in controls. Interestingly, the carrier of one of these variants also harbored two mutations in the Parkin gene. None of the carriers had atypical features previously described in patients with two mutated ATP13A2 alleles (Kufor-Rakeb syndrome). Our data suggest that two mutated ATP13A2 alleles are not a common cause of PD. Although heterozygous variants are present in a considerable number of patients, they are - based on this relatively small sample -

Materias

ATP13A2

Heterozygous changes

Neuroimaging

Parkinson's disease

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