Circular RNA CDR1as Exerts Oncogenic Properties Partially through Regulating MicroRNA 641 in Cholangiocarcinoma
Dingyang Li, Zhe Tang, Zhiqiang Gao, Pengcheng Shen, Zhaochen Liu, Xiaowei Dang
Abstract
Additionally, CDR1as expression was inversely correlated with miR-641 in CCA cells, and miR-641 could directly bind with CDR1as and its target genes, the AKT3 and mTOR genes. Mechanistically, CDR1as could bind with miR-641 and accelerate miR-641 degradation, which possibly leads to the upregulation of the relative mRNA levels of AKT3 and mTOR in RBE cells. In conclusion, our findings indicated that CDR1as might exert oncogenic properties, at least partially, by regulating miR-641 in CCA. CDR1as and miR-641 could be considered therapeutic targets for CCA.
Topics & Concepts
BiologymicroRNACircular RNARNACell biologyCancer researchGeneticsGeneCircular RNAs in diseasesMicroRNA in disease regulationCancer-related molecular mechanisms research