: We investigated the role of copy number variations (CNVs) in Parkinson's disease (PD) using genotyping data from 10,815 patients (2731 early-onset PD, EOPD) and 8901 controls from the COURAGE-PD consortium. CNVs were analyzed using a sliding window genome-wide association and burden approach. No genome-wide significant CNVs were detected in the overall cohort, but a robust deletion spanning exons 2-6 of PRKN was identified in EOPD cases, validated by MLPA, and replicated in the GP2 dataset (23,089 cases, 18,824 controls). CNV burden was significantly enriched in PD-related genes, primarily driven by PRKN, with the strongest effect observed in EOPD. PRKN CNV carriers showed earlier age at onset, confirmed by survival analysis. No association was observed for genome-wide or large CNV burden. Our findings reinforce the pivotal role of PRKN deletions in early-onset PD and highlight the need for high-resolution CNV analysis in large cohorts to uncover additional rare contributors to PD risk.

Genome-wide association study of copy number variations in Parkinson's disease / Landoulsi, Z., Sreelatha, A.A.K., Kuznetsov, N., Schulte, C., Bobbili, D.R., Montanucci, L., Leu, C., Niestroj, L., Hassanin, E., Domenighetti, C., Sugier, P., Radivojkov-Blagojevic, M., Lichtner, P., Portugal, B., Edsall, C., Krüger, J., Hernandez, D.G., Blauwendraat, C., Mellick, G.D., Zimprich, A., et al.. - In: NPJ PARKINSON'S DISEASE. - ISSN 2373-8057. - (2026). [10.1038/s41531-025-01245-z]

Genome-wide association study of copy number variations in Parkinson's disease

Valente, Enza Maria;Petrucci, Simona;Vitale, Dan;
2026

Abstract

: We investigated the role of copy number variations (CNVs) in Parkinson's disease (PD) using genotyping data from 10,815 patients (2731 early-onset PD, EOPD) and 8901 controls from the COURAGE-PD consortium. CNVs were analyzed using a sliding window genome-wide association and burden approach. No genome-wide significant CNVs were detected in the overall cohort, but a robust deletion spanning exons 2-6 of PRKN was identified in EOPD cases, validated by MLPA, and replicated in the GP2 dataset (23,089 cases, 18,824 controls). CNV burden was significantly enriched in PD-related genes, primarily driven by PRKN, with the strongest effect observed in EOPD. PRKN CNV carriers showed earlier age at onset, confirmed by survival analysis. No association was observed for genome-wide or large CNV burden. Our findings reinforce the pivotal role of PRKN deletions in early-onset PD and highlight the need for high-resolution CNV analysis in large cohorts to uncover additional rare contributors to PD risk.
2026
genome-wide association study; copy number variations; Parkinson's disease
01 Pubblicazione su rivista::01a Articolo in rivista
Genome-wide association study of copy number variations in Parkinson's disease / Landoulsi, Z., Sreelatha, A.A.K., Kuznetsov, N., Schulte, C., Bobbili, D.R., Montanucci, L., Leu, C., Niestroj, L., Hassanin, E., Domenighetti, C., Sugier, P., Radivojkov-Blagojevic, M., Lichtner, P., Portugal, B., Edsall, C., Krüger, J., Hernandez, D.G., Blauwendraat, C., Mellick, G.D., Zimprich, A., et al.. - In: NPJ PARKINSON'S DISEASE. - ISSN 2373-8057. - (2026). [10.1038/s41531-025-01245-z]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1766969
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