FAXDC2 inhibits the proliferation and invasion of human liver cancer HepG2 cells.

IF 2.4 4区 医学 Q3 MEDICINE, RESEARCH & EXPERIMENTAL
Zhilin Peng, Siting Xu, Qing Zhang, Xueting Yang, Wuzhou Yuan, Yuequn Wang, Yongqing Li, Ping Zhu, Xiushan Wu, Zhigang Jiang, Fang Li, Xiongwei Fan
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Abstract

The reprogramming of lipid metabolism serves an important role in occurrence and development of liver cancer. Fatty acid hydroxylase domain containing 2 (FAXDC2) is a hydroxylase involved in the synthesis of cholesterol and sphingomyelin and downregulated in various types of cancer. There are no reports on the relationship between FAXDC2 and liver carcinogenesis. The present study used multiple portals and publicly available tools to explore its correlation with liver cancer. The results showed that the expression of FAXDC2 decreased in liver cancer and the methylation level near the promoter increased. Patients with liver cancer and with low expression of FAXDC2 had a poor prognosis. Gain of function and loss of function strategies were performed to evaluate its roles in liver cancer cells. CCK-8 assay showed that overexpression of FAXDC2 inhibited the viability of liver cancer cells (HepG2). Flow cytometry analysis indicated that HepG2 cells with overexpressing FAXDC2 showed an S phase arrest, associated with cyclin-dependent kinase 2 decreased. Transwell experiments showed that increasing FAXDC2 inhibited HepG2 cell invasion ability, accompanied by the upregulation of E-cadherin. Notably, knockdown of FAXDC2 had no significant effect on cell cycle and invasion functions. Based on the cBioPortal platform, FAXDC2 was predicted to closely correlate to the ERK signal in tumorigenesis. Western blotting results showed that overexpression of FAXDC2 decreased the phosphorylation level of ERK in liver cancer cells. The present study first identified FAXDC2 as a liver cancer suppressor, which might inhibit the proliferation and invasion of liver cancer cells through the mechanism associated with ERK signaling. The present study provided a possible new target for the diagnosis and treatment of liver cancer.
FAXDC2 可抑制人肝癌 HepG2 细胞的增殖和侵袭。
脂质代谢的重编程在肝癌的发生和发展中起着重要作用。含脂肪酸羟化酶结构域 2(FAXDC2)是一种羟化酶,参与胆固醇和鞘磷脂的合成,在多种癌症中被下调。目前还没有关于FAXDC2与肝癌发生关系的报道。本研究利用多种门户网站和公开工具探讨其与肝癌的相关性。结果显示,FAXDC2在肝癌中的表达量降低,启动子附近的甲基化水平升高。FAXDC2低表达的肝癌患者预后较差。为了评估FAXDC2在肝癌细胞中的作用,研究人员采用了功能获得和功能丧失策略。CCK-8检测表明,FAXDC2的过表达抑制了肝癌细胞(HepG2)的活力。流式细胞术分析表明,过表达FAXDC2的HepG2细胞出现S期停滞,与细胞周期蛋白依赖性激酶2的减少有关。Transwell实验表明,FAXDC2的增加抑制了HepG2细胞的侵袭能力,并伴随着E-cadherin的上调。值得注意的是,敲除FAXDC2对细胞周期和侵袭功能没有明显影响。基于cBioPortal平台,FAXDC2被预测与肿瘤发生过程中的ERK信号密切相关。Western印迹结果显示,过表达FAXDC2可降低肝癌细胞中ERK的磷酸化水平。本研究首次发现FAXDC2是一种肝癌抑制因子,它可能通过与ERK信号相关的机制抑制肝癌细胞的增殖和侵袭。本研究为肝癌的诊断和治疗提供了一个可能的新靶点。
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来源期刊
Experimental and therapeutic medicine
Experimental and therapeutic medicine MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
1.50
自引率
0.00%
发文量
570
审稿时长
1 months
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