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Behavioral screening defines three molecular Parkinsonism subgroups in Drosophila

Output Details

Preprint August 28, 2024

Published March 9, 2026

Parkinsonism is defined by motor dysfunction, but the specific upstream molecular causes of these clinical symptoms can vary widely. We hypothesize that these causes converge onto a limited number of core cellular pathways. To investigate this, we created a new collection of 24 genetically very well-controlled animal models of familial forms of parkinsonism. Using unbiased behavioral screening and machine learning we identified three clusters of mutants that converge on (1) mitochondrial function; (2) retromer/vesicle trafficking; and (3) proteostasis/autophagy. Genes within each cluster have a similar genetic interaction profile and compounds that target specific molecular pathways ameliorate dopaminergic neuron dysfunction in a cluster-specific manner. This suggests that familial parkinsonism can be stratified into three broad functional groups and our findings pave the way for targeted biomarker discovery and drug development.
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  • Original Research

Meet the Authors

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    Natalie Kaempf

    External Collaborator

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    Jorge De Sousa Valadas

    External Collaborator

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    Pieter Robberechts

    External Collaborator

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    Nils Schoovaerts

    External Collaborator

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    Roman Praschberger

    External Collaborator

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    Antonio Ortega

    External Collaborator

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    Ayse Kilic

    External Collaborator

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    Dries Chabot

    External Collaborator

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    Ulrike Pech

    External Collaborator

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    Sabine Kuenen

    External Collaborator

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    Sven Vilain

    External Collaborator

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    El-Sayed Baz

    External Collaborator

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    Jeevanjot Singh

    External Collaborator

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    Jesse Davis

    External Collaborator

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    Sha Liu

    External Collaborator

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    Patrik Verstreken

    External Collaborator

Aligning Science Across Parkinson's
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