Roberto A. Ortega scite author profile

; for the LRRK2 Ashkenazi Jewish Consortium IMPORTANCE Few prospective longitudinal studies have evaluated the progression of Parkinson disease (PD) in patients with the leucine-rich repeat kinase 2 (LRRK2 [OMIM 609007]) mutation. Knowledge about such progression will aid clinical trials. OBJECTIVE To determine whether the longitudinal course of PD in patients with the LRRK2 mutation differs from the longitudinal course of PD in patients without the mutation.

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Digitized Spiral Drawing: A Possible Biomarker for Early Parkinson’s Disease

Luciano

Wang

Ortega

et al. 2016

PLoS ONE

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IntroductionPre-clinical markers of Parkinson’s Disease (PD) are needed, and to be relevant in pre-clinical disease, they should be quantifiably abnormal in early disease as well. Handwriting is impaired early in PD and can be evaluated using computerized analysis of drawn spirals, capturing kinematic, dynamic, and spatial abnormalities and calculating indices that quantify motor performance and disability. Digitized spiral drawing correlates with motor scores and may be more sensitive in detecting early changes than subjective ratings. However, whether changes in spiral drawing are abnormal compared with controls and whether changes are detected in early PD are unknown.Methods138 PD subjects (50 with early PD) and 150 controls drew spirals on a digitizing tablet, generating x, y, z (pressure) data-coordinates and time. Derived indices corresponded to overall spiral execution (severity), shape and kinematic irregularity (second order smoothness, first order zero-crossing), tightness, mean speed and variability of spiral width. Linear mixed effect adjusted models comparing these indices and cross-validation were performed. Receiver operating characteristic analysis was applied to examine discriminative validity of combined indices.ResultsAll indices were significantly different between PD cases and controls, except for zero-crossing. A model using all indices had high discriminative validity (sensitivity = 0.86, specificity = 0.81). Discriminative validity was maintained in patients with early PD.ConclusionSpiral analysis accurately discriminates subjects with PD and early PD from controls supporting a role as a promising quantitative biomarker. Further assessment is needed to determine whether spiral changes are PD specific compared with other disorders and if present in pre-clinical PD.

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Dysregulation of mitochondrial and proteolysosomal genes in Parkinson’s disease myeloid cells

et al. 2021

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Association of Dual LRRK2 G2019S and GBA Variations With Parkinson Disease Progression

et al. 2021

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Roberto A. Ortega

Progression in the LRRK2-Associated Parkinson Disease Population

Digitized Spiral Drawing: A Possible Biomarker for Early Parkinson’s Disease

Dysregulation of mitochondrial and proteolysosomal genes in Parkinson’s disease myeloid cells

Association of Dual LRRK2 G2019S and GBA Variations With Parkinson Disease Progression

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