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Long non‐coding <scp>RNA</scp> uc.80‐ overexpression promotes <scp>M2</scp> polarization of microglias to ameliorate depression in rats

Xunhu Gu, Lijun Xu, Li‐Li Zheng, Yuan‐Jian Yang, Zhenyu Tang, Han‐Jun Wu, Zhenzhen Chen, Wei Wang

2020IUBMB Life21 citationsDOIOpen Access PDF

Abstract

Microglia polarization is associated with the pathogenesis of depression. A previous study shows that long non-coding RNA uc.80- is down-regulated in the hippocampus of depressed rats. Thus, this article aims to investigate the role of uc.80- in microglia polarization in depression. We first established depression model rats by chronic unpredictable mild stress (CUMS) regiment. We found that hippocampus of depressed rats exhibited an increase of M1 microglias and a decrease of M2 microglias. uc.80- was down-regulated in hippocampus of depressed rats. Furthermore, the detection of behaviouristics of depressed rats showed that uc.80- overexpression alleviated depression of rats. In addition, uc.80- overexpression promoted M2 polarization of microglias in vivo and in vitro. uc.80- overexpression led to a decrease in apoptosis of hippocampal neurons in vivo and in vitro. In conclusion, our study confirms that lncRNA uc.80- overexpression ameliorates depression in rats by promoting M2 polarization of microglias. Thus, our work suggests that uc.80- may be a target gene for depression treatment.

Topics & Concepts

RNALong non-coding RNAPolarization (electrochemistry)ChemistryDownregulation and upregulationCell biologyCancer researchMedicineBiologyBiochemistryGenePhysical chemistryNeuroinflammation and Neurodegeneration MechanismsCancer-related molecular mechanisms researchImmune cells in cancer