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Propionic acid induces dendritic spine loss by MAPK/ERK signaling and dysregulation of autophagic flux

Authors
Choi, HyosunKim, In SikMun, Ji Young
Issue Date
Jun-2020
Publisher
BMC
Keywords
Propionic acid; Short-chain fatty acid; Autophagy; MAPK; ERK signaling; Spine density
Citation
MOLECULAR BRAIN, v.13, no.1
Journal Title
MOLECULAR BRAIN
Volume
13
Number
1
URI
http://scholarworks.bwise.kr/kbri/handle/2023.sw.kbri/609
DOI
10.1186/s13041-020-00626-0
ISSN
1756-6606
Abstract
Propionic acid (PPA) is a short-chain fatty acid that is an important mediator of cellular metabolism. It is also a by-product of human gut enterobacteria and a common food preservative. A recent study found that rats administered with PPA showed autistic-like behaviors like restricted interest, impaired social behavior, and impaired reversal in a T-maze task. This study aimed to identify a link between PPA and autism phenotypes facilitated by signaling mechanisms in hippocampal neurons. Findings indicated autism-like pathogenesis associated with reduced dendritic spines in PPA-treated hippocampal neurons. To uncover the mechanisms underlying this loss, we evaluated autophagic flux, a functional readout of autophagy, using relevant biomedical markers. Results indicated that autophagic flux is impaired in PPA-treated hippocampal neurons. At a molecular level, the mitogen-activated protein kinase (MAPK)/extracellular signal-regulated kinase (ERK) pathway was activated and autophagic activity was impaired. We also observed that a MAPK inhibitor rescued dendritic spine loss in PPA-treated hippocampal neurons. Taken together, these results suggest a previously unknown link between PPA and autophagy in spine formation regulation in hippocampal neurons via MAPK/ERK signaling. Our results indicate that MAPK/ERK signaling participates in autism pathogenesis by autophagy disruption affecting dendritic spine density. This study may help to elucidate other mechanisms underlying autism and provide a potential strategy for treating ASD-associated pathology.
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