4.6 Article

LncRNA CRART16/miR-122-5p/FOS axis promotes angiogenesis of gastric cancer by upregulating VEGFD expression

AGING-US (2022)

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Journal

AGING-US
Volume 14, Issue 9, Pages 4137-4157

Publisher

IMPACT JOURNALS LLC

Keywords

gastric cancer; angiogenesis; microRNA; long non-coding RNA; CRART16

Categories

Cell Biology Geriatrics & Gerontology

Funding

  1. National Key R&D Program of China [2020YFC2008304]
  2. Project of National MDT Capacity Construction for Serious Diseases
  3. National Natural Science Foundation of China [81641098]
  4. 'Sanming' medicine Project of Shenzhen City
  5. Youth Clinical Research Project of Peking University First Hospital [2018CR23, 2021CR03]
  6. Scientific Research Seed Fund of Peking University First Hospital [2018SF090]
  7. Youth Cultivated Research Fund of Peking University Health Center [BMU2020PYB026]

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CRART16 is highly expressed in gastric cancer tissues and correlates with advanced tumor stages and poor prognosis. It promotes angiogenesis in gastric cancer by downregulating miR-122-5p, upregulating FOS, and increasing VEGFD expression.
Background: We previously identified a novel lncRNA, CRART16, that could induce cetuximab resistance in colorectal cancer cells. This study explored the relationship of CRART16 expression to gastric cancer progression and the molecular mechanisms involved. Methods: We evaluated CRART16 expression in gastric cancer tissues and adjacent normal tissues from the TCGA database and our hospital. Besides, we assessed its relationship with the overall survival (OS) of patients with gastric cancer. The effects of CRART16 on gastric cancer angiogenesis were determined by endothelial tube formation assay, spheroid sprouting assay, HUVEC invasion assay, and chick embryo chorioallantoic membrane (CAM) assay. The involvement of the lncRNA CRART16/miR-122-5p/FOS axis was analyzed by western blotting and dual-luciferase reporter assay. The functions of CRART16 were confirmed in xenograft mouse models. Results: We found that CRART16 was substantially overexpressed in gastric cancer tissues compared with normal tissues, based on the TCGA database and our clinical samples. High expression of CRART16 correlated with more advanced tumor stages and poor prognosis. Overexpression of CRART16 in gastric cancer cells promoted proliferation, colony formation, angiogenesis, and bevacizumab resistance in vitro, and it promoted tumor growth and angiogenesis in vivo, and vice versa. CRART16 was found to downregulate miR-122-5p by acting as a sponge, upregulating the target oncogene FOS. Afterward, the increased FOS expression led to the upregulation of VEGFD. Conclusion: Our findings demonstrate that CRART16 promotes angiogenesis in vitro and in vivo, and CRART16 is a prognostic marker and therapeutic target in gastric cancer.

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