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LRRK2-Associated Parkinsonism With and Without In Vivo Evidence of Pathologic Alpha-Synuclein: Clinical and Biomarker Characterization

L. Chahine, D. Lafontant, C. Choi, H. Iwaki, M. Brumm, R. Alcalay, K. Nudelman, A. Dagher, K. Merchant, A. Vo, Q. Tao, C. Venuto, K. Kieburtz, K. Poston, S. Bressman, P. Gonzalez Latapi, B. Avants, C. Coffey, D. Jennings, E. Tolosa, A. Siderowf, K. Marek, T. Simuni (Pittsburgh, USA)

Meeting: 2024 International Congress

Abstract Number: 930

Keywords: , ,

Category: Parkinson's Disease: Molecular Mechanisms of Disease

Objective: To compare clinical and biomarker features and rate of progression among LRRK2-associated parkinsonism cases with and without in vivo evidence of pathologic alpha-synuclein (asyn) in cerebrospinal fluid (CSF).

Background: Among LRRK2-associated parkinsonism cases with nigral degeneration, over two-thirds demonstrate evidence of abnormal asyn, but a substantial minority do not. Understanding the clinical phenotype and underlying biology in such individuals is critical for molecularly-targeted therapeutic development.

Method: Data used in this analysis are from the Parkinson’s Progression Markers Initiative (PPMI; www.ppmi-info.com). The sample includes LRRK2-associated parkinsonism, age and disease-duration frequency-matched sporadic PD, and healthy control groups. Presence of pathologic CSF asyn was assessed with the asyn seed amplification assay (SAA). A range of clinician- and patient- reported outcome assessments were administered. Olfaction was assessed with smell identification test and hyposmia defined as ≤15th percentile expected for age and sex.  Biomarkers included dopamine transporter (DAT) scan, CSF amyloid-beta1-42, total tau, phospho-tau, and neurofilament light chain. To investigate possible genetic modifiers, the groups were compared with polygenic risk score analysis and risk variant analysis.

Results: The sample included 148 LRRK2-parkinsonism cases (86% G2019S variant), 46 SAA- and 102 SAA+ cases. At baseline, compared to the SAA+ group, the SAA- group were older (median [IQR] 61.5 [55.6-66.9] vs 69.1 [65.2-72.2] years, p<0.0001), more likely to be female (43 (42%) vs 28 (61%), p=0.035), and less likely to be hyposmic (75 (77%) vs 13 (29%), p<0.0001). Compared to the SAA+ group, the SAA- group had significantly higher percent expected DAT binding in the putamen for their age and sex (median [IQR] 0.26 [0.22-0.37] vs 0.36 [0.29-0.45], p<0.0001). Genetic analysis did not reveal significant differences in the 2 groups. A comparison of CSF biomarkers and longitudinal progression among the groups is underway.

Conclusion: We found clinical and biomarker differences in LRRK2-parkinsonism cases with in vivo evidence of pathologic asyn compared to those without. The underlying biology in LRRK2-parkinsonism cases without asyn requires further investigation to inform therapeutic development.

To cite this abstract in AMA style:

L. Chahine, D. Lafontant, C. Choi, H. Iwaki, M. Brumm, R. Alcalay, K. Nudelman, A. Dagher, K. Merchant, A. Vo, Q. Tao, C. Venuto, K. Kieburtz, K. Poston, S. Bressman, P. Gonzalez Latapi, B. Avants, C. Coffey, D. Jennings, E. Tolosa, A. Siderowf, K. Marek, T. Simuni. LRRK2-Associated Parkinsonism With and Without In Vivo Evidence of Pathologic Alpha-Synuclein: Clinical and Biomarker Characterization [abstract]. Mov Disord. 2024; 39 (suppl 1). https://www.mdsabstracts.org/abstract/lrrk2-associated-parkinsonism-with-and-without-in-vivo-evidence-of-pathologic-alpha-synuclein-clinical-and-biomarker-characterization/. Accessed June 14, 2025.

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