Literature DB >> 27904670

eIF5A2 is an alternative pathway for cell proliferation in cetuximab-treated epithelial hepatocellular carcinoma.

Fei Xue1, Yanhui Liu1, Haoyuan Chu1, Yu Wen1, Lei Yan1, Qiang Tang1, Erhui Xiao1, Dongyi Zhang1, Hongwei Zhang1.   

Abstract

Heaptocellular carcinoma (HCC) is still a great health problem around the world. Recently, the cetuximab has been implicated to have therapeutic values for HCC. However, cetuximab-resistance has also been synchronously reported pertaining to HCC treatment. This study aimed to evaluate the role of eIF5A2 in cetuximab-treated HCC cell proliferation, and whether eIF5A2 specific inhibitor GC7 has any effects on cetuximab-mediated proliferation inhibition in HCC cell lines. It was observed that GC7 significantly inhibited cell proliferation in HCC cell lines. GC7 synergized cetuximab to inhibit the proliferation in epithelial HCC cell lines HepG2, Huh7 and Hep3B, but not in mesenchymal cell lines SNU387 and SNU449. Knockdown of eIF5A-2 by specific siRNA exhibited the similar effects as GC7 did. In cetuximab-treated cells, cetuximab decreased the protein level of EGFR and phosphorylated STAT3 and unexpectedly up-regulated the expression level of eIF5A2, indicating the activation of eIF5A2 pathway. In turn, cetuximab also synergized GC7 to inhibit cell proliferation in epithelial cell lines. GC7 also suppressed hypoxia-induced cell proliferation in epithelial cell lines. These data suggest that eIF5A2 is an alternative pathway for cell proliferation in epithelial HCC cells escaping from the cytotoxicity of cetuximab. The eIF5A inhibitor GC7 might be a potent agent that promotes the cytotoxicity of cetuximab on epithelial HCC cells.

Entities:  

Keywords:  Cetuximab; GC7; eIF5A; hepatocellular carcinoma

Year:  2016        PMID: 27904670      PMCID: PMC5126312     

Source DB:  PubMed          Journal:  Am J Transl Res            Impact factor:   4.060


  25 in total

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  9 in total

1.  Long non‑coding RNA HOTTIP promotes hepatocellular carcinoma tumorigenesis and development: A comprehensive investigation based on bioinformatics, qRT‑PCR and meta‑analysis of 393 cases.

Authors:  Yu Zhang; Jia-Cheng Huang; Kai-Teng Cai; Xi-Bing Yu; You-Rong Chen; Wen-Ya Pan; Ze-Liang He; Jun Lv; Zhen-Bo Feng; Gang Chen
Journal:  Int J Oncol       Date:  2017-10-16       Impact factor: 5.650

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Authors:  Yuexiao Tang; Ke Chen; Xiaorui Luan; Jinyan Zhang; Rongrong Liu; Xiaoxiao Zheng; Shangzhi Xie; Haiping Ke; Xianning Zhang; Wei Chen
Journal:  Int J Oncol       Date:  2020-11-02       Impact factor: 5.650

3.  linc‑ROR facilitates hepatocellular carcinoma resistance to doxorubicin by regulating TWIST1‑mediated epithelial‑mesenchymal transition.

Authors:  Yuanbiao Zhang; Weiding Wu; Qiang Sun; Longyun Ye; Dongkai Zhou; Weilin Wang
Journal:  Mol Med Rep       Date:  2021-03-24       Impact factor: 2.952

4.  Circ_0003998 enhances doxorubicin resistance in hepatocellular carcinoma by regulating miR-218-5p/EIF5A2 pathway.

Authors:  Xiaomin Li; Jiefeng He; Xiaojing Ren; Haichao Zhao; Haoliang Zhao
Journal:  Diagn Pathol       Date:  2020-12-11       Impact factor: 2.644

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Authors:  Jing Ai; Junhui Sun; Guanhui Zhou; Tongyin Zhu; Li Jing
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Authors:  Weiwei Tang; Ziyi Chen; Wenling Zhang; Ye Cheng; Betty Zhang; Fan Wu; Qian Wang; Shouju Wang; Dawei Rong; F P Reiter; E N De Toni; Xuehao Wang
Journal:  Signal Transduct Target Ther       Date:  2020-06-10

8.  FIBCD1 overexpression predicts poor prognosis in patients with hepatocellular carcinoma.

Authors:  Yan Wang; Mengjing Sun; Jibin Liu; Ying Liu; Chunyi Jiang; Huijun Zhu; Wei Wang; Yao Wang
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Review 9.  STAT3 signaling in ovarian cancer: a potential therapeutic target.

Authors:  Renba Liang; Xishan Chen; Li Chen; Fangzhu Wan; Kaihua Chen; Yongchu Sun; Xiaodong Zhu
Journal:  J Cancer       Date:  2020-01-01       Impact factor: 4.207

  9 in total

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