Gly-tRF enhances LCSC-like properties and promotes HCC cells migration by targeting NDFIP2

Background Accumulating evidence demonstrates that tRFs (tRNA-derived small RNA fragments) and tiRNAs (tRNA-derived stress-induced RNA), an emerging category of regulatory RNA molecules derived from transfer RNAs (tRNAs), are dysregulated in in various human cancer types and play crucial roles. Howe...

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Published in:Cancer cell international 2021-09, Vol.21 (1), p.1-502, Article 502
Main Authors: Zhou, Yongqiang, Hu, Jinjing, Liu, Lu, Yan, Mengchao, Zhang, Qiyu, Song, Xiaojing, Lin, Yan, Zhu, Dan, Wei, Yongjian, Fu, Zongli, Hu, Liming, Chen, Yue, Li, Xun
Format: Article
Language:English
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3' Untranslated regions
AKT
AKT protein
Antibodies
Cell adhesion & migration
Cell migration
EMT
Experiments
Flow cytometry
Gene expression
Hepatocellular carcinoma
Hepatocytes
Life sciences
Liver cancer
Liver cancer stem cells
Medical prognosis
Mesenchyme
mRNA
NDFIP2
Primary Research
Signal transduction
Stem cells
Therapeutic targets
Transfer RNA
tRNA Gly
tRNA-derived fragments
Tumor cell lines
Tumors
Western blotting
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Summary:Background Accumulating evidence demonstrates that tRFs (tRNA-derived small RNA fragments) and tiRNAs (tRNA-derived stress-induced RNA), an emerging category of regulatory RNA molecules derived from transfer RNAs (tRNAs), are dysregulated in in various human cancer types and play crucial roles. However, their roles and mechanisms in hepatocellular carcinoma (HCC) and liver cancer stem cells (LCSCs) are still unknown. Methods The expression of glycine tRNA-derived fragment (Gly-tRF) was measured by qRT-PCR. Flow cytometric analysis and sphere formation assays were used to determine the properties of LCSCs. Transwell assays and scratch wound assays were performed to detect HCC cell migration. Western blotting was conducted to evaluate the abundance change of Epithelial-mesenchymal transition (EMT)-related proteins. Dual luciferase reporter assays and signalling pathway analysis were performed to explore the underlying mechanism of Gly-tRF functions. Results Gly-tRF was highly expressed in HCC cell lines and tumour tissues. Gly-tRF mimic increased the LCSC subpopulation proportion and LCSC-like cell properties. Gly-tRF mimic promoted HCC cell migration and EMT. Loss of Gly-tRF inhibited HCC cell migration and EMT. Mechanistically, Gly-tRF decreased the level of NDFIP2 mRNA by binding to the NDFIP2 mRNA 3′ UTR. Importantly, overexpression of NDFIP2 weakened the promotive effects of Gly-tRF on LCSC-like cell sphere formation and HCC cell migration. Signalling pathway analysis showed that Gly-tRF increased the abundance of phosphorylated AKT. Conclusions Gly-tRF enhances LCSC-like cell properties and promotes EMT by targeting NDFIP2 and activating the AKT signalling pathway. Gly-tRF plays tumor-promoting role in HCC and may lead to a potential therapeutic target for HCC.
ISSN:1475-2867
1475-2867
DOI:10.1186/s12935-021-02102-8