Subthalamic stimulation may inhibit the beneficial effects of levodopa on akinesia and gait

Subthalamic stimulation may inhibit the beneficial effects of levodopa on akinesia and gait

Background Gait and akinesia deterioration in PD patients during the immediate postoperative period of DBS has been directly related to stimulation in the subthalamic region. The underlying mechanisms remain poorly understood. The aim of the present study was to clinically and anatomically describe...

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Veröffentlicht in:Movement disorders 2016-09, Vol.31 (9), p.1389-1397
Hauptverfasser: Fleury, Vanessa, Pollak, Pierre, Gere, Julien, Tommasi, Giorgio, Romito, Luigi, Combescure, Christophe, Bardinet, Eric, Chabardes, Stephan, Momjian, Shahan, Krainik, Alexandre, Burkhard, Pierre, Yelnik, Jérôme, Krack, Paul
Format: Artikel
Sprache:eng
Schlagworte:
Adult
Aged
Combined Modality Therapy
Deep Brain Stimulation - adverse effects
Dopamine Agents - administration & dosage
Dopamine Agents - pharmacology
Dyskinesias - etiology
Female
Gait Disorders, Neurologic - etiology
Humans
Levodopa - administration & dosage
Levodopa - pharmacology
Male
Middle Aged
Movement disorders
Parkinson Disease - drug therapy
Parkinson Disease - therapy
Subthalamic Nucleus
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Zusammenfassung:Background Gait and akinesia deterioration in PD patients during the immediate postoperative period of DBS has been directly related to stimulation in the subthalamic region. The underlying mechanisms remain poorly understood. The aim of the present study was to clinically and anatomically describe this side effect. Methods PD patients presenting with a worsening of gait and/or akinesia following STN‐DBS, that was reversible on stimulation arrest were included. The evaluation included (1) a Stand Walk Sit Test during a monopolar survey of each electrode in the on‐drug condition; (2) a 5‐condition test with the following conditions: off‐drug/off‐DBS, off‐drug/on‐best‐compromise‐DBS, on‐drug/off‐DBS, on‐drug/on‐best‐compromise‐DBS, and on‐drug/on‐worsening‐DBS, which utilized the contact inducing the most prominent gait deterioration. The following scales were performed: UPDRSIII subscores, Stand Walk Sit Test, and dyskinesia and freezing of gait scales. Localization of contacts was performed using a coregistration method. Results Twelve of 17 patients underwent the complete evaluation. Stimulation of the most proximal contacts significantly slowed down the Stand Walk Sit Test. The on‐drug/on‐worsening‐DBS condition compared with the on‐drug/off‐DBS condition worsened akinesia (P = 0.02), Stand Walk Sit Test (P = 0.001), freezing of gait (P = 0.02), and improved dyskinesias (P = 0.003). Compared with the off‐drug/off‐DBS condition, the on‐drug/on‐worsening‐DBS condition improved rigidity (P = 0.007) and tremor (P = 0.007). Worsening contact sites were predominantly dorsal and anterior to the STN in the anterior zona incerta and Forel fields H2. Conclusions A paradoxical deterioration of gait and akinesia is a rare side effect following STN‐DBS. We propose that this may be related to misplaced contacts, and we discuss the pathophysiology and strategies to identify and manage this complication. © 2016 International Parkinson and Movement Disorder Society
ISSN:0885-3185
1531-8257
DOI:10.1002/mds.26545