Background: The outcome of levodopa/carbidopa intestinal gel (LCIG) in Parkinson's disease carriers of GBA1 mutations (GBA-PD) remains uncertain. Objective: To evaluate the safety and efficacy of LCIG in a large PD cohort, focusing on GBA1 variants. Methods: This multicenter, retrospective, longitudinal “real-world” study included consecutive patients with advanced PD treated with LCIG at 31 Italian centers; data were collected at baseline, 1-, 5-year, and last-available follow-up. Results: Data from 512 PD patients (59% male, mean age and disease duration at LCIG initiation 67.0 ± 8.0 and 12.9 ± 5.0 years, respectively) were analyzed. GBA1 genotyping was available for 306 patients (60%), of whom 40 (13%) had GBA1 mutations or risk variants. Mean follow-up on LCIG was 3.9 ± 2.9 years; 5-year follow-up data were available for 159 subjects. At baseline, GBA-PD had a younger age, shorter PD duration, worse cognition, and more hallucinations than noncarriers. At 1- and 5-year follow-up, LCIG improved motor and non-motor symptoms, OFF-time, and dyskinesias in the entire population. In GBA-PD, MDS-UPDRS parts I, II, and III scores did not change, while part IV score improved significantly less than in noncarriers; cognition and orthostatic hypotension symptoms worsened more rapidly. Multivariate analysis of predictors for adverse events and LCIG discontinuation found no significant contribution from GBA1 mutation status. Conclusions: GBA1 status does not increase the risk of adverse events or LCIG discontinuation. LCIG is a safe option for advanced GBA-PD, even in patients with cognitive impairment at baseline. However, GBA-PD experiences lower efficacy on motor disability and complications and faster cognitive decline than noncarriers.
Effects of GBA1 Variants in Patients With Parkinson's Disease and Levodopa-Carbidopa Intestinal Gel: A Nation-Wide, Multicenter, Longitudinal, "Real-World" Study. The EPIC Study / R. Cilia, F. Colucci, E. Cereda, A.E. Elia, V. Leta, S. Barca, M. Zibetti, M. Carecchio, S. Bonvegna, G. Calandra-Buonaura, R. Cerroni, R. De Micco, S. Tamburin, L. Magistrelli, F. Lena, M.M. Mascia, M. Picillo, G. Cossu, M. Marano, A. Zampogna, C. Pellicano, V. Fioravanti, A. Pilotto, R. Zangaglia, M. Avenali, C. Sorbera, F. Di Biasio, F. Arienti, A. Nicoletti, C. Bagella, M.C. Malaguti, A. Ranghetti, E. Caputo, D. Alimonti, E. Torre, G.D. Oggioni, C. Leuzzi, L.M. Romito, N.G. Andreasi, G. Devigili, R. Telese, A. Braccia, G. Gaudiano, S. Mazzetti, F. Invernizzi, B. Garavaglia, G. Imbalzano, C. Ledda, P. Antenucci, A. Gozzi, G. Bonato, M. Percetti, G. Giannini, L. Sambati, T. Schirinzi, M. D'Anna, D. Rinaldi, F. Cavallieri, M. Liccari, A. Priori, M. Sessa, F. Tamma, M. Canesi, P. Solla, M. Zappia, A. Di Fonzo, L. Avanzino, A. Quartarone, E.M. Valente, C. Pacchetti, A. Padovani, F. Valzania, F.E. Pontieri, A. Suppa, M.T. Pellecchia, N. Modugno, C. Comi, M. Tinazzi, A. Tessitore, A. Stefani, P. Cortelli, I.U. Isaias, A. Antonini, M. Sensi, L. Lopiano, R. Eleopra. - In: EUROPEAN JOURNAL OF NEUROLOGY. - ISSN 1468-1331. - 32:7(2025 Jul), pp. e70179.1-e70179.18. [10.1111/ene.70179]
Effects of GBA1 Variants in Patients With Parkinson's Disease and Levodopa-Carbidopa Intestinal Gel: A Nation-Wide, Multicenter, Longitudinal, "Real-World" Study. The EPIC Study
M. Percetti;A. Priori;
2025
Abstract
Background: The outcome of levodopa/carbidopa intestinal gel (LCIG) in Parkinson's disease carriers of GBA1 mutations (GBA-PD) remains uncertain. Objective: To evaluate the safety and efficacy of LCIG in a large PD cohort, focusing on GBA1 variants. Methods: This multicenter, retrospective, longitudinal “real-world” study included consecutive patients with advanced PD treated with LCIG at 31 Italian centers; data were collected at baseline, 1-, 5-year, and last-available follow-up. Results: Data from 512 PD patients (59% male, mean age and disease duration at LCIG initiation 67.0 ± 8.0 and 12.9 ± 5.0 years, respectively) were analyzed. GBA1 genotyping was available for 306 patients (60%), of whom 40 (13%) had GBA1 mutations or risk variants. Mean follow-up on LCIG was 3.9 ± 2.9 years; 5-year follow-up data were available for 159 subjects. At baseline, GBA-PD had a younger age, shorter PD duration, worse cognition, and more hallucinations than noncarriers. At 1- and 5-year follow-up, LCIG improved motor and non-motor symptoms, OFF-time, and dyskinesias in the entire population. In GBA-PD, MDS-UPDRS parts I, II, and III scores did not change, while part IV score improved significantly less than in noncarriers; cognition and orthostatic hypotension symptoms worsened more rapidly. Multivariate analysis of predictors for adverse events and LCIG discontinuation found no significant contribution from GBA1 mutation status. Conclusions: GBA1 status does not increase the risk of adverse events or LCIG discontinuation. LCIG is a safe option for advanced GBA-PD, even in patients with cognitive impairment at baseline. However, GBA-PD experiences lower efficacy on motor disability and complications and faster cognitive decline than noncarriers.
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