Litcius/Paper detail

LINC00662 sponges miR-107 accelerating the invasiveness and proliferation of glioma cells

Jinsong Wu, Xiaolong Guo, Dongxiao Xu, Hongri Zhang

2020Journal of Cancer17 citationsDOIOpen Access PDF

Abstract

Increasing evidence revealed that the aberrant expression of long non-coding RNAs (lncRNAs) has been implicated in tumorigenesis. However, the role and mechanisms of LINC00662 in glioma have not been elucidated. Here, we show that upregulation of LINC00662 expression in glioma is associated with advanced clinical features and poor prognosis. Our results from loss-of-function assays suggest that LINC00662 silencing suppresses the proliferative and invasive abilities of glioma cells. In vivo, glioma growth was inhibited by depletion of LINC00662 in nude mice. Mechanistically, LINC00662 directly interacts with miR-107. The High-mobility group box 1 protein (HMGB1) is a known target of miR-107. Moreover, rescue assays reveal that HMGB1 overexpression (or miR-107 inhibition) reverses the glioma growth inhibition caused by LINC00662 knockdown. In conclusion, our results indicate that LINC00662 acts as an oncogene in glioma by modulating the miR-107/HMGB1 axis, suggesting that LINC00662 could be a novel therapeutic target for glioma treatment.

Topics & Concepts

GliomaGene knockdownGene silencingDownregulation and upregulationCancer researchOncogeneCarcinogenesisIn vivoBiologymicroRNAHMGB1ChemistryCell cultureImmunologyCellCancerGeneGeneticsCell cycleInflammationCancer-related molecular mechanisms researchCircular RNAs in diseasesMicroRNA in disease regulation
LINC00662 sponges miR-107 accelerating the invasiveness and proliferation of glioma cells | Litcius