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miR-21a-5p Promotes Inflammation following Traumatic Spinal Cord Injury through Upregulation of Neurotoxic Reactive Astrocyte (A1) Polarization by Inhibiting the CNTF/STAT3/Nkrf Pathway

Yining Zhang, Ting-Ting Meng, Jianan Chen, Ying Zhang, Jianning Kang, Xinyu Li, Guilian Yu, Lige Tian, Zhengxin Jin, Hui Dong, Xiaodi Zhang, Bin Ning

2021International Journal of Biological Sciences52 citationsDOIOpen Access PDF

Abstract

Reactive astrocytes are implicated in traumatic spinal cord injury (TSCI). Interestingly, nave astrocytes can easily transform into neurotoxic reactive astrocytes (A1s) with inflammatory stimulation. Previous studies demonstrated that microRNA(miR)-21a-5p was up-regulated in spinal cord tissue after TSCI; however, it is not clear whether this affected reactive astrocyte polarization. Here, we aim to detect the effects of miR-21a-5p on the induction of A1 formation and the underlying mechanisms. Our study found that the expression of miR-21a-5p was significantly increased while that of Cntfr was decreased, since nave astrocytes transformed into A1s 3 days post-TSCI; the binding site between miR-21a-5p and Cntfr was further confirmed in astrocytes. After treatment with CNTF, the levels of A1 markers decreased while that of A2 increased. The expression of A1 markers significantly decreased with the downregulation of miR-21a-5p, while Cntfr siRNA treatment caused the opposite both in vitro and in vivo. To summarize, miR-21a-5p/Cntfr promotes A1 induction and might enhance the inflammatory process of TSCI; furthermore, we identified, for the first time, the effect and potential mechanism by which CNTF inhibits nave astrocytes transformation into A1s. Collectively, our findings demonstrate that targeting miR-21a-5p represents a prospective therapy for promoting the recovery of TSCI.

Topics & Concepts

AstrocyteDownregulation and upregulationCiliary neurotrophic factorChemistrySTAT3InflammationStimulationSpinal cord injuryIn vivoSpinal cordCell biologyPharmacologyBiologyNeuroscienceMedicineInternal medicineBiochemistryCentral nervous systemSignal transductionNeurotrophic factorsReceptorGeneBiotechnologySpinal Cord Injury ResearchNeuroinflammation and Neurodegeneration MechanismsNeurogenesis and neuroplasticity mechanisms
miR-21a-5p Promotes Inflammation following Traumatic Spinal Cord Injury through Upregulation of Neurotoxic Reactive Astrocyte (A1) Polarization by Inhibiting the CNTF/STAT3/Nkrf Pathway | Litcius