4.4 Article

Reduced Short-Latency Afferent Inhibition in Parkinson's Disease Patients with L-dopa-Unresponsive Freezing of Gait

期刊

JOURNAL OF PARKINSONS DISEASE
卷 12, 期 8, 页码 2507-2518

出版社

IOS PRESS
DOI: 10.3233/JPD-223498

关键词

Freezing of gait; cholinergic activity; pedunculopontine nucleus; short-latency afferent inhibition; transcranial magnetic stimulation; Parkinson's disease

资金

  1. National Natural Science Foundation of China [81671258]
  2. Jiangsu Social Development Project [BE2022808]

向作者/读者索取更多资源

This study found that reduced cortical sensorimotor inhibition (SAI) is associated with severe freezing of gait (FOG) manifestations, impaired gait characteristics, and variability in PD patients with L-dopa-unresponsive FOG. This suggests the involvement of impaired thalamocortical cholinergic-GABAergic SAI pathways in ONOFF-FOG.
Background: Freezing of gait (FOG) in Parkinson's disease (PD), especially the L-dopa-unresponsive subtype, is associated with the dysfunction of non-dopaminergic circuits. Objective: We sought to determine whether cortical sensorimotor inhibition evaluated by short-latency afferent inhibition (SAI) related to cholinergic and gamma-aminobutyric acid (GABA)-ergic activities is impaired in PD patients with L-dopaunresponsive FOG (ONOFF-FOG). Methods: SAI protocol was performed in 28 PD patients with ONOFF-FOG, 15 PD patients with off FOG (OFF-FOG), and 25 PD patients without FOG during medication on state. Additionally, 10 ONOFF-FOG patients underwent SAI testing during both off and on states. Twenty healthy controls participated in this study. Gait was measured objectively using a portable Inertial Measurement Unit system, and participants performed 5-meter Timed Up and Go single- and dual-task conditions. Spatiotemporal gait characteristics and their variability were determined. FOG manifestations and cognition were assessed with clinical scales. Results: Compared to controls, PD patients withoutFOGand with OFF-FOG, ONOFF-FOG PD patients showed significantly reduced SAI. Further, dopaminergic therapy had no remarkable effect on this SAI alterations in ONOFF-FOG. Meanwhile, OFF-FOG patients presented decreased SAI only relative to controls. PD patients with ONOFF-FOG exhibited decreased gait speed, stride length, and increased gait variability relative to PD patients without FOG and controls under both walking conditions. For ONOFF-FOG patients, significant associations were found between SAI and FOG severity, gait characteristics and variability. Conclusion: Reduced SAI was associated with severe FOG manifestations, impaired gait characteristics and variability in PD patients with ONOFF-FOG, suggesting the impaired thalamocortical cholinergic-GABAergic SAI pathways underlying ONOFF-FOG.

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