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Effects of cancer-testis antigen TFDP3 on cell cycle regulation and its mechanism in L-02 and HepG2 cell lines in vitro

机译:睾丸抗原TFDP3对L-02和HepG2细胞系体外细胞周期调控及其机制的影响

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摘要

TFDP3, also be known as HCA661, was one of the cancer-testis antigens, which only expressed in human tissues. The recent researches about TFDP3 mostly focused on its ability to control the drug resistance and apoptosis of tumor cells. However, the role of TFDP3 in the progress of the cell cycle is rarely involved. In this study, we examined the expression of TFDP3 in human liver tissues firstly. After that, we detect the expression of TFDP3 at the RNA level and protein level in L-02 cell line and HepG2 cell line, and the location of TFDP3 was defined by immunofluorescence technique. Furthermore, we synchronized the cells to G1 phase, S phase and G2 phase, and arrested cell mitosis. The localization of TFDP3 and co-localization with E2F1 molecules in different phases of hepatocyte lines. Finally, TFDP3 gene knockout was performed on L-02 and HepG2 cell lines, and detected the new cell cycles by flow cytometry. The result showed that the expression of TFDP3 molecule is negative in normal liver tissue, but positive in immortalized human hepatocyte cell line, and the expression level is lower than in hepatocellular carcinoma cell line. The expression level of TFDP3 was in the dynamic change of L-02 and HepG2 cell lines, and was related to the phase transition. TFDP3 can bind to E2F1 molecule to form E2F/TFDP3 complex; and the localizations of TFDP3 and E2F1 molecules and the co-localization were different in different phases of cell cycle in the nucleus and cytoplasm, which indicated that the E2F/TFDP3 complex involved in the process of regulating the cell cycle. By knocking down the TFDP3 expression level in L-02 and HepG2 cell lines, the cell cycle would be arrested in S phase, which confirmed that TFDP3 can be a potential target for tumor therapy.
机译:TFDP3,也称为HCA661,是仅在人类组织中表达的癌-睾丸抗原之一。关于TFDP3的最新研究主要集中在其控制肿瘤细胞的耐药性和凋亡的能力上。但是,很少涉及TFDP3在细胞周期进程中的作用。在这项研究中,我们首先检查了人肝组织中TFDP3的表达。之后,我们检测了L-02细胞系和HepG2细胞系中TFDP3在RNA和蛋白质水平的表达,并通过免疫荧光技术确定了TFDP3的位置。此外,我们将细胞同步至G1期,S期和G2期,并阻止了细胞的有丝分裂。 TFDP3的定位和与E2F1分子在肝细胞系不同阶段的共定位。最后,对L-02和HepG2细胞系进行了TFDP3基因敲除,并通过流式细胞术检测了新的细胞周期。结果表明,TFDP3分子在正常肝组织中表达为阴性,而在永生化的人肝细胞系中为阳性,且表达水平低于肝细胞癌细胞系。 TFDP3的表达水平与L-02和HepG2细胞系的动态变化有关,并且与相变有关。 TFDP3可与E2F1分子结合形成E2F / TFDP3复合物; TFDP3和E2F1分子的定位以及共定位在细胞周期的不同阶段在细胞核和细胞质中是不同的,这表明E2F / TFDP3复合物参与了细胞周期的调控过程。通过敲低L-02和HepG2细胞系中的TFDP3表达水平,细胞周期将被阻滞在S期,这证实TFDP3可能是肿瘤治疗的潜在靶标。

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