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circRNA rtcisE2F regulates the self-renewal of liver tumor-initiating cell by crosstalking with RNA m6A modification

04.08.22 | Science China Press

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The molecular mechanism of rtcisE2F.
rt-circRNA rtcisE2F is originated from two adjacent genes CYP2C18 and CYP2C19, involves in the binding between m6A E2F6/E2F3 mRNAs and m6A readers IGF2BP2/YTHDF2, and finally promotes the stability of E2F6/E2F3 mRNAs. E2F6 and E2F3 drive the activation of Wnt/β-catenin signaling and the self-renewal of liver TICs. Credit: ©Science China Press

Liver cancer is one of the most serious tumors in China. Tumor-initiating cells (TICs), a small subset cells in tumor bulk with self-renewal and differentiation capacities, play key roles in tumor formation, metastasis, drug resistance and recurrence. circRNAs, formed by covalent conjugation of 5’ and 3’ ends through backsplicing, play important regulatory roles in many physiological and pathological processes. However, the role of circRNAs in liver cancer and TICs needs further study.

Recently, groups of Pingping Zhu (School of Life Sciences, Zhengzhou University) and Benyu Liu (The Academy of Medical Science, Zhengzhou University) have identified a circrNA, termed rtcisE2F, is highly expressed in liver TICs. rtcisE2F plays an essential role in the self-renewal of liver TICs. rtcisE2F targets E2F6 and E2F3 mRNAs, attenuates mRNA turnover, and increases E2F6/E2F3 expression. Mechanistically, rtcisE2F functions as a scaffold of m 6 A reader IGF2BP2 and m 6 A modified E2F6/E2F3 mRNA. rtcisE2F promotes the association of E2F6/E2F3 mRNAs with IGF2BP2, and inhibits their association with another m 6 A reader, YTHDF2. IGF2BP2 inhibits E2F6/E2F3 mRNA decay, whereas YTHDF2 promotes E2F6/E2F3 mRNA decay. By switching m 6 A readers, rtcisE2F enhances E2F6/E2F3 mRNA stability. E2F6 and E2F3 are both required for liver TIC self-renewal and Wnt/β-catenin activation, and inhibition of these pathways is a potential strategy for preventing liver tumorigenesis and metastasis.

Although there have been some studies on the roles of m 6 A modification and circRNAs in tumorigenesis and tumor metastasis, there have been few reports on the interaction between m 6 A modification and circRNA, and systematic studies on the interaction between m 6 A and circRNA in liver tumor and TICs are still lacking. The new findings of Pingping Zhu and Benyu Liu reveal that circRNA play a key role in the binding of m 6 A modified mRNA to different m 6 A readers. The rtcisE2F -IGF2BP2 /YTHDF2-E2F6/E2F3-Wnt/β-catenin pathway has been found for the first time to drive the self-renewal of liver TICs, and the tumorgenesis and metastasis of HCC as well. Moreover, these discoveries may provide an additional strategy to eliminate liver TICs.

The work is published in Science China Life Sciences, and the raw article is linked below.

https://link.springer.com/article/10.1007/s11427-021-2038-5

Science China Life Sciences

10.1007/s11427-021-2038-5

3-Mar-2022

Keywords

Health and Medicine Life Sciences

Article Information

Journal
Science China Life Sciences
DOI
10.1007/s11427-021-2038-5
Article Publication Date
2022-03-03

Contact Information

Bei Yan
Science China Press
yanbei@scichina.org

How to Cite This Article

APA:
Science China Press. (2022, April 8). circRNA rtcisE2F regulates the self-renewal of liver tumor-initiating cell by crosstalking with RNA m6A modification. Brightsurf News. https://www.brightsurf.com/news/1WRN3YML/circrna-rtcise2f-regulates-the-self-renewal-of-liver-tumor-initiating-cell-by-crosstalking-with-rna-m6a-modification.html
MLA:
"circRNA rtcisE2F regulates the self-renewal of liver tumor-initiating cell by crosstalking with RNA m6A modification." Brightsurf News, Apr. 8 2022, https://www.brightsurf.com/news/1WRN3YML/circrna-rtcise2f-regulates-the-self-renewal-of-liver-tumor-initiating-cell-by-crosstalking-with-rna-m6a-modification.html.