Effect of Early Levodopa Treatment on Mortality in People with Parkinson's Disease

Author:

Talebi Amir H.1ORCID,Darweesh Sirwan K.L.1ORCID,Bloem Bas R.1,Bucur Ioan G.2,Heskes Tom2

Affiliation:

1. Radboud University Medical Centre, Donders Institute for Brain, Cognition and Behaviour, Department of Neurology Center of Expertise for Parkinson & Movement Disorders Nijmegen The Netherlands

2. Data Science Research Department, Institute for Computing and Information Sciences Radboud University Nijmegen The Netherlands

Abstract

AbstractBackgroundThe ideal timing for initiating levodopa in newly diagnosed people with Parkinson's disease (PD) is uncertain due to limited data on the long‐term effects of levodopa.ObjectiveThe aim was to investigate whether early levodopa initiation postpones mortality (primary outcome), the requirement of device‐aided therapies, and the incidence of PD‐related complications, such as fall‐induced injuries.MethodsUsing nationwide claims data from Dutch hospitals (2012–2020), we grouped newly diagnosed PD individuals as “early initiators” (initiating levodopa within 2 years of diagnosis) or “nonearly initiators.” We used the national death registry to assess mortality and health‐care claims to assess PD‐related complications and device‐aided therapies. We used marginal structural models to compare mortality and device‐aided therapy rates between groups, and a Poisson regression model to compare PD‐related complication rates.ResultsAmong 29,943 newly diagnosed PD individuals (mean age at diagnosis: 71.6, 38.5% female), there were 24,847 early and 5096 nonearly levodopa initiators. Over a median 4.25 years, 8109 (27.1%) died. The causal risk ratio for mortality was 1.04 (95% confidence interval [CI] 0.92–1.19) for early versus nonearly initiators. The risk ratio of receiving any device‐aided therapy was 3.19 (95% CI 2.56–5.80). No association was observed with incidence of PD‐related complications (incidence rate ratio: 1.00, 95% CI 0.96–1.05).ConclusionsEarly levodopa initiation in PD does neither postpone nor accelerate mortality or PD‐related complications, nor does it precipitate earlier occurrence of PD‐related complications or mortality. However, we cannot exclude that the results were influenced by residual confounding due to unmeasured risk factors of mortality.

Funder

Gatsby Charitable Foundation

Publisher

Wiley

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