| Literature DB >> 32052431 |
Ping Wan1, Xuan Bai1, Chao Yang1, Tian He1, Lilin Luo1, Yun Wang1, Minmin Fan1, Zhilin Wang1, Liming Lu1, Yajing Yin1, Sisi Li1, Qiang Guo1, Zhengyi Song1.
Abstract
microRNAs (miRNAs), a kind of small noncoding RNAs, are considered able to regulate expression of genes and mediate RNA silencing. miR-129-5p was shown to be a cancer-related miRNA. However, the influence of miR-129-5p in rectal adenocarcinoma (READ) development remains to be determined. Based on the TCGA data, downregulation of miR-129-5p in READ samples was observed. Manual restoration of the miR-129-5p in SW1463 and SW480 cell lines significantly inhibited invasion, migration, and proliferation of READ cell lines, while the apoptosis ability was enhanced. Meanwhile, we found E2F7 acted as a potential target of miR-129-5p and was upregulated in READ samples. E2F7 upregulation reversed the repression of miR-129-5p on READ development. Finally, in vivo experiments showed that inhibition of tumor growth in nude mice was achieved through upregulating miR-129-5p. Overall, our findings suggest increasing of miR-129-5p leads to the suppression of READ progression through regulating the expression of E2F7, which may provide novel insights into the treatment of READ.Entities:
Keywords: E2F7; miR-129-5p; rectal adenocarcinoma
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Year: 2020 PMID: 32052431 DOI: 10.1002/jcp.29501
Source DB: PubMed Journal: J Cell Physiol ISSN: 0021-9541 Impact factor: 6.384