miR-873-5p inhibits the progression of colon cancer via repression of tumor suppressor candidate 3/AKT signaling
Yufeng Zhu, Xiaojian Zhang, Ming Qi, Yong Zhang, Feng Ding
Journal:JOURNAL OF GASTROENTEROLOGY AND HEPATOLOGY
IF:3.63
DOI:10.1111/jgh.14697
PMID:31039290
Published:2019-04-30
research field:免疫学传染病学材料科学纳米医学
Abstract
Background and Aim We previously discovered that tumor suppressor candidate 3 (TUSC3) was overexpressed and predicted worse prognosis in colon cancer patients. However, the mechanisms of upregulation of TUSC3 in colon cancer remained unclear. Methods MiR-873-5p was predicted and identified as the regulator of TUSC3 via online programs and luciferase reporter assays. The roles of miR-873-5p in regulating colon cancer cell proliferation, colony formation, and invasion were evaluated in vitro . Animal studies were performed to investigate the effects of miR-873-5p on proliferation and lung metastasis. Moreover, the miR-873-5p/TUSC3 related signaling pathway and the prognostic value of combining miR-873-5p and TUSC3 for colon cancer patients were also explored. Results Here, we identified miR-873-5p as a novel regulator of TUSC3 in colon cancer. Functionally, ectopic expression or silencing of miR-873-5p, respectively, inhibited or promoted colon cancer cells proliferation, colony formation, and invasion, as well as prevented or enhanced the metastasis of colon cancer cells in vitro and in vivo . Molecularly, miR-873-5p functioned as a tumor suppressor by inhibiting the TUSC3/AKT pathway. Overexpression or silencing of TUSC3 could partially reverse the effects of the overexpression or repression of miR-873-5p on colon cancer progression caused by activation of the AKT pathway. Clinically, low miR-873-5p expression predicted poor survival in colon cancer patients, especially combined with high TUSC3 expression. Conclusions We identified miR-873-5p as a tumor suppressor, which acts by directly repressing TUSC3 in colon cancer.
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