miR-100a-5p-enriched exosomes derived from mesenchymal stem cells enhance the anti-oxidant effect in a Parkinson's disease model via regulation of Nox4/ROS/Nrf2 signaling.

Songzhe HeQiongqiong WangLiankuai ChenYusheng Jason HeXiaofang WangShaogang Qu

Published in: Journal of translational medicine (2023)

The study suggests that miR-100-5p-enriched T-MSCs-Exo may be a promising biological agent for the treatment of PD. Schematic summary of the mechanism underlying the neuroprotective actions of T-MSCs-Exo in PD. T-MSCs Exo may inhibit the expression level of the target gene NOX4 by delivering miR-100-5p, thereby reducing ROS production and alleviating oxidative stress via the Nox4-ROS-Nrf2 axis, thus improving DA neuron damage in PD.

Keyphrases

mesenchymal stem cells
reactive oxygen species
oxidative stress
umbilical cord
dna damage
cell death
bone marrow
cell therapy
ischemia reperfusion injury
induced apoptosis
stem cells
dna methylation
genome wide
gene expression
transcription factor
cerebral ischemia
replacement therapy
genome wide identification