E2F3 promotes cancer growth and is overexpressed through copy number variation in human melanoma

E2F3 促进癌症生长,并通过人类黑色素瘤中的拷贝数变异过度表达

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作者:Zhicai Feng, Cheng Peng, Daojiang Li, Danhua Zhang, Xu Li, Fengran Cui, Yanhong Chen, Quanyong He

Conclusion

It can be speculated that copy number amplification and other mechanisms result in the high expression of E2F3 in melanoma, which promotes tumor progression by involving the cell cycle. E2F3 is a good target for the treatment of melanoma.

Results

We found that E2F3 showed extensive copy number amplification that was positively correlated with the expression level. Patients with high copy number had a significantly poorer prognosis. We also found that E2F3 levels were significantly negatively correlated with promoter methylation. However, we showed that the E2F3 promoter region is hypomethylated, and in normal cells or tumor cells, the methylation level did not correlate with expression. Finally, we knocked down the E2F3 gene in melanoma cells by shRNA. Colony formation, anchorage-dependent growth, and EdU cell proliferation experiments showed a significant decrease in proliferation. Flow cytometry showed a significant increase in the G0/G1 ratio.

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