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Protein-protein interaction networks identify targets which rescue the MPP+ cellular model of Parkinson's disease

Abstract:
Neurodegenerative diseases are complex multifactorial disorders characterised by the interplay of many dysregulated physiological processes. As an exemplar, Parkinson's disease (PD) involves multiple perturbed cellular functions, including mitochondrial dysfunction and autophagic dysregulation in preferentially-sensitive dopamine neurons, a selective pathophysiology recapitulated in vitro using the neurotoxin MPP +. Here we explore a network science approach for the selection of therapeutic protein targets in the cellular MPP + model. We hypothesised that analysis of protein-protein interaction networks modelling MPP + toxicity could identify proteins critical for mediating MPP + toxicity. Analysis of protein-protein interaction networks constructed to model the interplay of mitochondrial dysfunction and autophagic dysregulation (key aspects of MPP + toxicity) enabled us to identify four proteins predicted to be key for MPP + toxicity (P62, GABARAP, GBRL1 and GBRL2). Combined, but not individual, knockdown of these proteins increased cellular susceptibility to MPP + toxicity. Conversely, combined, but not individual, over-expression of the network targets provided rescue of MPP + toxicity associated with the formation of autophagosome-like structures. We also found that modulation of two distinct proteins in the protein-protein interaction network was necessary and sufficient to mitigate neurotoxicity. Together, these findings validate our network science approach to multi-target identification in complex neurological diseases.
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.1038/srep17004

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More by this author
Institution:
University of Oxford
Division:
MSD
Department:
Physiology Anatomy & Genetics
Role:
Author
More by this author
Institution:
University of Oxford
Division:
MSD
Department:
Psychiatry
Role:
Author
More by this author
Institution:
University of Oxford
Division:
MSD
Department:
Physiology Anatomy & Genetics
Role:
Author

Contributors

Jackson, B


Publisher:
Nature Publishing Group
Journal:
Scientific Reports More from this journal
Volume:
5
Publication date:
2015-11-26
DOI:
EISSN:
2045-2322
ISSN:
2045-2322


Pubs id:
pubs:579554
UUID:
uuid:1344a510-77e9-4e2b-8833-7a4e3b8b2c96
Local pid:
pubs:579554
Source identifiers:
579554
Deposit date:
2015-12-13
ARK identifier:

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