4.3 Article

LncRNA DANCR regulates lymphatic metastasis of bladder cancer via the miR-335/VEGF-C axis

TRANSLATIONAL ANDROLOGY AND UROLOGY (2021)

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Journal

TRANSLATIONAL ANDROLOGY AND UROLOGY
Volume 10, Issue 4, Pages -

Publisher

AME PUBL CO
DOI: 10.21037/tau-21-226

Keywords

Bladder cancer; DANCR; miR-335; VEGF-C; lymphatic metastasis

Categories

Andrology Urology & Nephrology

Funding

  1. Basic Research Project of Yunnan Provincial: Kunming Medical University Joint Special Project [2018FE001090]
  2. Medical Discipline Leader Project of Yunnan Provincial [D-2017044]
  3. Open Project from the Tumor Immunization and Prevention Key Experiment Laboratory of Yunnan Provincial [2017DG00404]
  4. Scientific Research Fund from the Education Department of Yunnan Provincial [2020J0218]
  5. Health Science and Technology Talent Training Project of Kunming City [2020-SW-12]
  6. Health Research Project from the Kunming Municipal Health Commission [2020-04-05-011]

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The study found that DANCR regulates the proliferation, migration, invasion, and lymphatic metastasis of bladder cancer cells through the miR-335/VEGF-C molecular axis. Inhibition of miR-335 and overexpression of VEGF-C can reverse the inhibitory effect of silencing DANCR on bladder cancer cells.
Background: Substantial evidence indicate that long non-coding RNA (lncRNA) and microRNA (miRNA) act as key role in bladder cancer. Differentiation antagonistic ncRNA (DANCR) could be used as a biomarker in the occurrence and development of cancer. This study aims to explore the mechanism of DANCR/miR-335/VEGF-C axis affecting lymphatic metastasis of bladder cancer. Methods: qRT-PCR detects the expression of DANCR in bladder cancer cell lines (SW780, 5637, T24, UM-UC-3) and normal bladder cell lines (SV-HUC-1), and selects T24 cell lines for subsequent experiments. The expression levels of DANCR, miR-335 and VEGF were measured by qRT-PCR, and the dual luciferase reporter gene verified the targeted regulation of DANCR on miR-335 and miR-335 on VEGF. CCK-8, Transwell and Wound healing assay detect the proliferation, invasion and migration ability of bladder cancer cells, Endothelial cell adhesion assay and Western blot further prove the lymphatic metastasis of bladder cancer. Results: In this study, DANCR was highly expressed in bladder cancer cell lines. Transfection of siDANCR significantly inhibits the proliferation, migration, invasion and lymphatic metastasis of bladder cancer cells. Dual luciferase assay confirmed that DANCR targets miR-335/VEGF-C. Transfection of miR-335 mimic promotes the proliferation, migration, invasion and lymphatic metastasis of bladder cancer cells, overexpression of DANCR eliminates the promotion of miR-335 mimic on bladder cancer cells. Further experiments proved that inhibition of miR-335 and overexpression of VEGF-C can reverse the inhibitory effect of silencing DANCR on bladder cancer cells. Conclusions: In bladder cancer, DARCR plays an important role, which regulates the proliferation, migration, invasion and lymphatic metastasis of bladder cancer cells through the miR-335/VEGF-C molecular axis.

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