| Literature DB >> 31197654 |
Marcela J Ramirez-Moreno1, Ana P Duarte-Jurado1, Yareth Gopar-Cuevas1, Alfredo Gonzalez-Alcocer1, Maria J Loera-Arias1, Odila Saucedo-Cardenas1,2, Roberto Montes de Oca-Luna1, Humberto Rodriguez-Rocha1, Aracely Garcia-Garcia3.
Abstract
The neurodegenerative process of Parkinson's disease (PD) involves autophagy impairment and oxidative stress. Therefore, we wanted to determine whether stimulation of autophagy protects dopaminergic cell death induced by oxidative stress in a PD model. Since environmental exposure to herbicides increases the risk to develop PD, the experimental model was established using the herbicide paraquat, which induces autophagy disruption, oxidative stress, and cell death. Rapamycin-stimulated autophagy inhibited calpain-dependent and independent apoptosis induced by paraquat. Autophagy stimulation decreased oxidative stress and peroxiredoxins (PRXs) hyperoxidation induced by paraquat. Cells exposed to paraquat displayed abnormally large autophagosomes enclosing mitochondria, which correlates with an increase of p62, an essential mitophagy regulator. Interestingly, when autophagy was stimulated before paraquat treatment, autophagosome size and number were similar to that observed in control cells. Motor and cognitive function impairment induced by paraquat showed an improvement when preceded by autophagy stimulation. Importantly, dopaminergic neuronal death and microglial activation mediated by paraquat were significantly reduced by rapamycin-induced autophagy. Our results indicate that autophagy stimulation has a protective effect on dopaminergic neurons and may have a promising potential to prevent or delay PD progression.Entities:
Keywords: Autophagy; Oxidative stress; Paraquat; Parkinson’s disease; Rapamycin
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Year: 2019 PMID: 31197654 DOI: 10.1007/s12035-019-01654-1
Source DB: PubMed Journal: Mol Neurobiol ISSN: 0893-7648 Impact factor: 5.590