Eye movement disorders are different in Parkin-linked and idiopathic early-onset PD
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Abstract
Objectives: Parkin gene mutations are the most common cause of early-onset parkinsonism. Patients with Parkin mutations may be clinically indistinguishable from patients with idiopathic early-onset Parkinson disease (EOPD) without Parkin mutations. Eye movement disorders have been shown to differentiate parkinsonian syndromes, but have never been systematically studied in Parkin mutation carriers.
Methods: Eye movements were recorded in symptomatic (n = 9) and asymptomatic Parkin mutation carriers (n = 13), patients with idiopathic EOPD (n = 14), and age-matched control subjects (n = 27) during established oculomotor tasks.
Results: Both patients with EOPD and symptomatic Parkin mutation carriers showed hypometric prosaccades toward visual stimuli, as well as deficits in suppressing reflexive saccades toward unintended targets (antisaccade task). When directing gaze toward memorized target positions, patients with EOPD exhibited hypometric saccades, whereas symptomatic Parkin mutation carriers showed normal saccades. In contrast to patients with EOPD, the symptomatic Parkin mutation carriers showed impaired tracking of a moving target (reduced smooth pursuit gain). The asymptomatic Parkin mutation carriers did not differ from healthy control subjects in any of the tasks.
Conclusions: Although clinically similarly affected, symptomatic Parkin mutation carriers and patients with idiopathic EOPD differed in several oculomotor tasks. This finding may point to distinct anatomic structures underlying either condition: dysfunctions of cortical areas involved in smooth pursuit (V5, frontal eye field) in Parkin-linked parkinsonism vs greater impairment of basal ganglia circuits in idiopathic Parkinson disease.
Footnotes
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Supplemental data at www.neurology.org
Study funding: B.M. was supported by the University Lübeck research grant E32–2008. A.S., C.H., and C.K. were supported by the project “Intermediate Phenotypes and Biomarkers,” Universities Lübeck and Kiel. C.K. is the recipient of grant support from the Hermann and Lilly Schilling Foundation, the Volkswagen Foundation, and the NGFN plus (Parkinson Network, Subproject 3: Recessive Parkinsonism PNP-01GS08135-3).
Disclosure: Author disclosures are provided at the end of the article.
Received November 3, 2009. Accepted in final form March 11, 2010.
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