Long-Term Safety and Clinical Effects of Nilotinib in Parkinson's Disease

Fernando L Pagan; Barbara Wilmarth; Yasar Torres-Yaghi; Michaeline L Hebron; Sanjana Mulki; Dalila Ferrante; Sara Matar; Jaeil Ahn; Charbel Moussa

doi:10.1002/mds.28389

Long-Term Safety and Clinical Effects of Nilotinib in Parkinson's Disease

Mov Disord. 2021 Mar;36(3):740-749. doi: 10.1002/mds.28389. Epub 2020 Nov 20.

Authors

Fernando L Pagan^{1

2}, Barbara Wilmarth^{1

2}, Yasar Torres-Yaghi^{1

2}, Michaeline L Hebron¹, Sanjana Mulki¹, Dalila Ferrante¹, Sara Matar¹, Jaeil Ahn³, Charbel Moussa¹

Affiliations

¹ Translational Neurotherapeutics Program, Laboratory for Dementia and Parkinsonism, Department of Neurology, Georgetown University Medical Center, Washington, District of Columbia, USA.
² Movement Disorders Clinic, Department of Neurology, MedStar Georgetown University Hospital, Washington, District of Columbia, USA.
³ Department of Biostatistics, Bioinformatics and Biomathematics, Georgetown University Medical Center, Washington, District of Columbia, USA.

Abstract

Background: Nilotinib is US Food and Drug Administration-approved for leukemia, and this open-label study investigated the safety, tolerability, and potential clinical effects of nilotinib in medically optimized patients with Parkinson's disease.

Objectives: Safety and tolerability were the primary objectives, and clinical outcomes were exploratory.

Methods: A total of 63 patients completed a 15-month phase 2, double-blind, placebo-controlled study and were rerandomized 1:1 into an open-label study of nilotinib 150 mg versus 300 mg for 12 months.

Results: Nilotinib was safe and tolerated, and no adverse effects seemed to be related to the drug, and no differences in adverse events were observed between groups. Exploratory clinical outcomes showed that nilotinib 300 mg was remarkably stable from baseline to 27 months using partial and total Unified Parkinson's Disease Scale (UPDRS). Nilotinib 150 mg versus 300 mg, significantly declined using partial or the sum of UPDRS Parts I and II. There was no significant difference in nilotinib 150 mg versus 300 mg using UPDRS Part III (on levodopa) and total UPDRS Parts I to III. Subgroup analysis showed that late-start nilotinib 150 mg significantly worsened using the sum of UPDRS Parts II + III and total UPDRS Parts I to III compared with late-start nilotinib 300 mg. Quality of life using the Parkinson's Disease Questionnaire in nilotinib 150 mg significantly declined between 15 and 27 months compared with nilotinib 300 mg, and there was no change in cognition using the Montreal Cognitive Assessment between groups.

Conclusions: This study provides evidence that nilotinib is safe and tolerated in Parkinson's disease. The exploratory clinical data will inform an adequately powered larger study to evaluate the efficacy of nilotinib 300 mg in Parkinson's disease. © 2020 The Authors. Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society.

Keywords: MoCA; Nilotinib; PDQ-39; Parkinson's disease; UPDRS.

Publication types

Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Antiparkinson Agents / adverse effects
Double-Blind Method
Humans
Levodopa
Parkinson Disease* / drug therapy
Pyrimidines
Quality of Life

Substances

Antiparkinson Agents
Pyrimidines
Levodopa
nilotinib