Department of General Surgery, Guangdong Second Provincial General Hospital, Guangzhou, China.
Department of General Surgery, Zengcheng People's Hospital, (BoJi-Affiliated Hospital of Sun Yat-Sen University), Zengcheng, China.
Neoplasma. 2018 Sep 19;65(5):701-707. doi: 10.4149/neo_2018_170725N503. Epub 2018 Jun 17.
The homology of epidermal growth factor receptor pathway substrate 8 (EPS8), EPS8L3, is elevated significantly in hepatocellular carcinoma (HCC) tissues and cell lines compared with the normal liver tissues and cell lines. The MTT and colony formation assays demonstrated that overexpressing EPS8L3 enhances, while silencing reduces the proliferation of HCC cells. Further experiments illustrated that overexpressing EPS8L3 promotes the expression of p-AKT, Cyclin D1, but inhibits the transcriptional activity of FOXO1. Besides, colony formation assay demonstrated that AKT inhibitor suppresses the effect of EPS8L3 on proliferation in EPS8L3-overexpressing cells, whereas AKT restores the proliferation of EPS8L3-silenced cells, suggesting that EPS8L3 might promote proliferation by hyperactivating the AKT signaling pathway and subsequently inhibiting the FOXO1 transcriptional activity. Our results provide new view between EPS8L3 and progression of human HCC, suggesting that EPS8L3 may be a novel therapeutic target for HCC.
表皮生长因子受体通路底物 8(EPS8)、EPS8L3 的同源性在肝癌(HCC)组织和细胞系中明显升高,与正常肝组织和细胞系相比。MTT 和集落形成实验表明,过表达 EPS8L3 增强,而沉默则降低 HCC 细胞的增殖。进一步的实验表明,过表达 EPS8L3 促进 p-AKT、Cyclin D1 的表达,但抑制 FOXO1 的转录活性。此外,集落形成实验表明,AKT 抑制剂抑制了 EPS8L3 在过表达 EPS8L3 细胞中的增殖作用,而 AKT 则恢复了 EPS8L3 沉默细胞的增殖,表明 EPS8L3 可能通过过度激活 AKT 信号通路并随后抑制 FOXO1 的转录活性来促进增殖。我们的研究结果为人类 HCC 中 EPS8L3 的作用提供了新的视角,提示 EPS8L3 可能成为 HCC 的一个新的治疗靶点。
