4.7 Article

Trehalose does not improve neuronal survival on exposure to alpha-synuclein pre-formed fibrils

Journal

REDOX BIOLOGY
Volume 11, Issue -, Pages 429-437

Publisher

ELSEVIER SCIENCE BV
DOI: 10.1016/j.redox.2016.12.032

Keywords

Parkinson's disease; Alpha-synuclein fibrils; P-alpha-synuclein trehalose; Autophagy; LC3-II

Funding

  1. [NIHR01-NS064090]

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Parkinson's disease is a debilitating neurodegenerative disorder that is pathologically characterized by intracellular inclusions comprised primarily of alpha-synuclein (alpha Syn) that can also be transmitted from neuron to neuron. Several lines of evidence suggest that these inclusions cause neurodegeneration. Thus exploring strategies to improve neuronal survival in neurons with alpha Syn aggregates is critical. Previously, exposure to alpha Syn pre-formed fibrils (PFFs) has been shown to induce aggregation of endogenous alpha Syn resulting in cell death that is exacerbated by either starvation or inhibition of mTOR by rapamycin, both of which are able to induce autophagy, an intracellular protein degradation pathway. Since mTOR inhibition may also inhibit protein synthesis and starvation itself can be detrimental to neuronal survival, we investigated the effects of autophagy induction on neurons with alpha Syn inclusions by a starvation and mTOR-independent autophagy induction mechanism. We exposed mouse primary cortical neurons to PFFs to induce inclusion formation in the presence and absence of the disaccharide trehalose, which has been proposed to induce autophagy and stimulate lysosomal biogenesis. As expected, we observed that on exposure to PFFs, there was increased abundance of pS129-alpha Syn aggregates and cell death. Trehalose alone increased LC3-II levels, consistent with increased autophagosome levels that remained elevated with PFF exposure. Interestingly, trehalose alone increased cell viability over a 14-d time course. Trehalose was also able to restore cell viability to control levels, but PFFs still exhibited toxic effects on the cells. These data provide essential information regarding effects of trehalose on aSyn accumulation and neuronal survival on exposure to PFF.

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