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Bidirectional regulation of levodopa-induced dyskinesia by a specific neural ensemble in globus pallidus external segment.


ABSTRACT: Levodopa-induced dyskinesia (LID) is an intractable motor complication arising in Parkinson's disease with the progression of disease and chronic treatment of levodopa. However, the specific cell assemblies mediating dyskinesia have not been fully elucidated. Here, we utilize the activity-dependent tool to identify three brain regions (globus pallidus external segment [GPe], parafascicular thalamic nucleus, and subthalamic nucleus) that specifically contain dyskinesia-activated ensembles. An intensity-dependent hyperactivity in the dyskinesia-activated subpopulation in GPe (GPeTRAPed in LID) is observed during dyskinesia. Optogenetic inhibition of GPeTRAPed in LID significantly ameliorates LID, whereas reactivation of GPeTRAPed in LID evokes dyskinetic behavior in the levodopa-off state. Simultaneous chemogenetic reactivation of GPeTRAPed in LID and another previously reported ensemble in striatum fully reproduces the dyskinesia induced by high-dose levodopa. Finally, we characterize GPeTRAPed in LID as a subset of prototypic neurons in GPe. These findings provide theoretical foundations for precision medication and modulation of LID in the future.

SUBMITTER: Shen C 

PROVIDER: S-EPMC11228392 | biostudies-literature | 2024 Jun

REPOSITORIES: biostudies-literature

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Bidirectional regulation of levodopa-induced dyskinesia by a specific neural ensemble in globus pallidus external segment.

Shen Cong C   Shen Bo B   Liu Dechen D   Han Linlin L   Zou Kexin K   Gan Linhua L   Ren Jingyu J   Wu Bin B   Tang Yilin Y   Zhao Jue J   Sun Yimin Y   Liu Fengtao F   Yu Wenbo W   Yao Haishan H   Wu Jianjun J   Wang Jian J  

Cell reports. Medicine 20240516 6


Levodopa-induced dyskinesia (LID) is an intractable motor complication arising in Parkinson's disease with the progression of disease and chronic treatment of levodopa. However, the specific cell assemblies mediating dyskinesia have not been fully elucidated. Here, we utilize the activity-dependent tool to identify three brain regions (globus pallidus external segment [GPe], parafascicular thalamic nucleus, and subthalamic nucleus) that specifically contain dyskinesia-activated ensembles. An int  ...[more]

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