Parallel roles of transcription factors dFOXO and FER2 in the development and maintenance of dopaminergic neurons

Autor: Rafael Koch, Emi Nagoshi, Luca Stickley, Bettina Gnägi, Damla Tas, Virginie Sabado, Federico Miozzo, Nicolas Loncle
Jazyk: angličtina
Rok vydání: 2018
Předmět:
0301 basic medicine
Cancer Research
Physiology
Biochemistry
Fats
Animal Cells
Medicine and Health Sciences
Basic Helix-Loop-Helix Transcription Factors
Drosophila Proteins
Genetics (clinical)
Energy-Producing Organelles
Neurons
Gene knockdown
Movement Disorders
Cell Death
Drosophila Melanogaster
Dopaminergic
Eukaryota
Neurodegenerative Diseases
Parkinson Disease
Forkhead Transcription Factors
Animal Models
Lipids
Climbing
Neuroprotection
Cell biology
Mitochondria
Insects
medicine.anatomical_structure
Neurology
Experimental Organism Systems
Cell Processes
Drosophila
Cellular Types
Cellular Structures and Organelles
Research Article
Programmed cell death
lcsh:QH426-470
Arthropoda
Cell Survival
Autophagic Cell Death
Biology
Bioenergetics
Research and Analysis Methods
03 medical and health sciences
Model Organisms
Genetics
medicine
Autophagy
Animals
Molecular Biology
Transcription factor
Ecology
Evolution
Behavior and Systematics
Loss function
Biological Locomotion
Dopaminergic Neurons
Organisms
Biology and Life Sciences
Cell Biology
Invertebrates
lcsh:Genetics
Oxidative Stress
030104 developmental biology
Cellular Neuroscience
Mutation
Neuron
Neuroscience
Zdroj: PLoS Genetics
PLoS Genetics, Vol 14, Iss 3, p e1007271 (2018)
ISSN: 1553-7404
1553-7390
Popis: Forkhead box (FOXO) proteins are evolutionarily conserved, stress-responsive transcription factors (TFs) that can promote or counteract cell death. Mutations in FOXO genes are implicated in numerous pathologies, including age-dependent neurodegenerative disorders, such as Parkinson’s disease (PD). However, the complex regulation and downstream mechanisms of FOXOs present a challenge in understanding their roles in the pathogenesis of PD. Here, we investigate the involvement of FOXO in the death of dopaminergic (DA) neurons, the key pathological feature of PD, in Drosophila. We show that dFOXO null mutants exhibit a selective loss of DA neurons in the subgroup crucial for locomotion, the protocerebral anterior medial (PAM) cluster, during development as well as in adulthood. PAM neuron-targeted adult-restricted knockdown demonstrates that dFOXO in adult PAM neurons tissue-autonomously promotes neuronal survival during aging. We further show that dFOXO and the bHLH-TF 48-related-2 (FER2) act in parallel to protect PAM neurons from different forms of cellular stress. Remarkably, however, dFOXO and FER2 share common downstream processes leading to the regulation of autophagy and mitochondrial morphology. Thus, overexpression of one can rescue the loss of function of the other. These results indicate a role of dFOXO in neuroprotection and highlight the notion that multiple genetic and environmental factors interact to increase the risk of DA neuron degeneration and the development of PD.
Author summary PD, mainly characterized by a progressive loss of dopaminergic neurons in the substantia nigra (SN), is the most prevalent neurodegenerative movement disorder affecting more than 6 million people worldwide. Despite the discovery of several genes linked to familial PD, our understanding of its pathogenesis remains limited, as approximately 90% of the PD cases are sporadic with no apparent genetic linkage. Genome-wide expression studies have implicated the stress-responsive TF FOXO in PD. However, the exact role of FOXO in the survival of DA neurons and PD pathogenesis is still poorly understood. Here, we use fruit flies to address the role of FOXO in the maintenance of DA neurons. dFOXO (Drosophila FOXO) null mutants show a progressive loss of DA neurons in the subgroup essential for locomotion, a phenotype identical to that of Fer2 mutants. Remarkably, dFOXO and FER2 act in parallel pathways to protect PAM neurons from different cellular stressors, but both pathways contribute to the regulation of autophagy and mitochondrial biology. These results demonstrate that dFOXO is required for the maintenance of DA neurons important for locomotion and shed new light on the molecular mechanisms underpinning the complex gene-environment interactions affecting DA neuron survival and PD pathogenesis.
Databáze: OpenAIRE
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