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RNA Editing Enzyme ADAR1 Suppresses the Mobility of Cancer Cells via ARPIN

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Abstract
Deamination of adenine or cytosine in RNA, called RNA editing, is a constitutively active and common modification. The primary role of RNA editing is tagging RNA right after its synthesis so that the endogenous RNA is recognized as self and distinguished from exogenous RNA, such as viral RNA. In addition to this primary function, the direct or indirect effects on gene expression can be utilized in cancer where a high level of RNA editing activity persists. This report identified actin-related protein 2/3 complex inhibitor (ARPIN) as a target of ADAR1 in breast cancer cells. Our comparative RNA sequencing analysis in MCF7 cells revealed that the expression of ARPIN was decreased upon ADAR1 depletion with altered editing on its 3'UTR. However, the expression changes of ARPIN were not dependent on 3'UTR editing but relied on three microRNAs acting on ARPIN. As a result, we found that the migration and invasion of cancer cells were profoundly increased by ADAR1 depletion, and this cellular phenotype was reversed by the exogenous ARPIN expression. Altogether, our data suggest that ADAR1 suppresses breast cancer cell mobility via the upregulation of ARPIN.
Issued Date
2023
Min Ji Park
Eunji Jeong
Eun Ji Lee
Hyeon Ji Choi
Bo Hyun Moon
Keunsoo Kang
Suhwan Chang
Type
Article
Keyword
ADAR1ARPINRNA editingbreast cancermetastasis
DOI
10.14348/molcells.2023.2174
URI
https://oak.ulsan.ac.kr/handle/2021.oak/17356
Publisher
MOLECULES AND CELLS
Language
영어
ISSN
1016-8478
Citation Volume
46
Citation Number
6
Citation Start Page
351
Citation End Page
359
Appears in Collections:
Medicine > Nursing
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