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Chinese Journal of Colorectal Diseases(Electronic Edition) ›› 2019, Vol. 08 ›› Issue (04): 383-389. doi: 10.3877/cma.j.issn.2095-3224.2019.04.011

Special Issue:

• Original Article • Previous Articles     Next Articles

The effect and mechanism of miRNA-1236 suppresses colorectal cancer cell proliferation by targeting FOXO3a

Yu Sun1, Lin Zhu1, Zhenlu Liu1, Ming Yang1, Zhen Yu1, Jing Sun1, Yan Wang1, Yuhan Jiang2, Hongyan Li3, Hui Sun4,()   

  1. 1. College of Pharmacy, Harbin Medical University, Harbin 150081, China
    2. College of Basic Medical, Harbin Medical University, Harbin 150081, China
    3. Traditional Chinese Medicine University of Heilongjiang, Harbin 150081, China
    4. College of Pharmacy, Harbin Medical University, Harbin 150081, China; Pharmaceutical Experiment Teaching Center, College of Pharmacy, Harbin Medical University, Harbin 150001, China
  • Received:2018-06-17 Online:2019-08-25 Published:2019-08-25
  • Contact: Hui Sun
  • About author:
    Corresponding author: Sun Hui, Email:

Abstract:

Objective

To investigate the role and mechanism of miRNA-1236 on proliferation in colorectal cancer.

Method

The expression of miRNA-1236 was detect by quantitative real-time PCR. The cell viability of HCT116 cells after transfected with miRNA-1236 was detected by CCK-8. The proliferation of miR-1236 in HCT116 cell was tested by colony formation assay and Ki67 staining. The potential target gene FOXO3a of miR-1236 was screened by bioinformatics. Observing the level of FOXO3a gene with transfection of miRNA-1236 by real-time quantitative PCR detection. Luciferase reports detected the binding site of miRNA-1236 with FOXO3a; The expression of FOXO3a in colorectal cancer was detected by immunohistochemistry. Detected the protein level of FOXO3a, PCNA and Bax in HCT116 cells after transfection with miR-1236 by western blotting. The expression of FOXO3a in colorectal Cancer-Para cancer patients with different cancer stages and genders was detected by TCGA database.

Results

The cell viability of HCT116 cells was significantly increased with the miRNA-1236 mimic compared with negative control group, while it was decreased with the miRNA-1236 inhibitor. The proliferation of HCT116 cells was significantly reduced compared with the negative control group by colony formation assay and Ki67 staining. Bioinformatics predicted potential binding sites between miR-1236 and FOXO3a. Using Western blot and quantitative real-time PCR of reverse transcription to verify that FOXO3a expression was significantly reduced after overexpression of miRNA-1236 than the negative control group, while FOXO3a expression was significantly increased after treat with miRNA-1236 inhibitor. Meanwhile, luciferase results showed that FOXO3a was a direct target gene of miRNA-1236. Simultaneously, FOXO3a was significantly reduced in colorectal cancer tissue.

Conclusion

miRNA-1236 regulate the proliferation of colorectal cancer by targeting FOXO3a, and significantly affects survival of colorectal cancer patients.

Key words: Colorectal neoplasms, miRNA-1236, FOXO3a, Proliferation

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