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Abnormal hyperactivity of specific striatal ensembles encodes distinct dyskinetic behaviors revealed by high-resolution clustering

Output Details

Preprint October 9, 2024

Published July 16, 2025

L-DOPA-induced dyskinesia (LID) is a debilitating complication of dopamine replacement therapy in Parkinsońs disease and the most common hyperkinetic disorder of basal ganglia origin. Abnormal activity of striatal D1 and D2 spiny projection neurons (SPNs) is critical for LID, yet the link between SPN activity patterns and specific dyskinetic movements remains unknown. To explore this, we developed a novel method for clustering movements based on high-resolution motion sensors and video recordings. In a mouse model of LID, this method identified two main dyskinesia types and pathological rotations, all absent during normal behavior. Using single-cell resolution imaging, we found that specific sets of both D1 and D2-SPNs were abnormally active during these pathological movements. Under baseline conditions, the same SPN sets were active during behaviors sharing physical features with LID movements. These findings indicate that ensembles of behavior-encoding D1- and D2-SPNs form new combinations of hyperactive neurons mediating specific dyskinetic movements.
Tags
  • Dopamine
  • Dopaminergic neurons
  • Dyskinesia
  • Levodopa
  • Neurobehavioral
  • Original Research

Meet the Authors

  • User avatar fallback logo

    Cristina Alcacer,

    External Collaborator

  • User avatar fallback logo

    Andreas Klaus

    External Collaborator

  • User avatar fallback logo

    Marcelo D Mendonça

    External Collaborator

  • User avatar fallback logo

    Sara F. Abalde

    External Collaborator

  • User avatar fallback logo

    Maria Angela Cenci

    External Collaborator

  • Rui Costa, PhD

    Co-PI (Core Leadership): Team Surmeier

    Allen Institute

Aligning Science Across Parkinson's
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