Over-expression and siRNA of a novel environmental lipopolysaccharide-responding gene on the cell cycle of the human hepatoma-derived cell line HepG2.

Du K; Chai Y; Hou L; Chang W; Chen S; Luo W; Cai T; Zhang X; Chen N; Chen Y; Chen J

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Over-expression and siRNA of a novel environmental lipopolysaccharide-responding gene on the cell cycle of the human hepatoma-derived cell line HepG2.

机译：一个新的环境脂多糖响应基因在人肝癌衍生细胞系HepG2的细胞周期中的过表达和siRNA。

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Lipopolysaccharide (LPS) is the toxic determinant for Gram-negative bacterium infection. The individual response to LPS was related to its gene background. It is necessary to identify new molecules and signaling transduction pathways about LPS. The present study was undertaken to evaluate the effects of a novel environmental lipopolysaccharide-responding (Elrg) gene on the regulation of proliferation and cell cycle of the hepatoma-derived cell line, HepG2. By means of RT-PCR, the new molecule of Elrg was generated from a human dental pulp cell cDNA library. Expression level of Elrg in HepG2 cells was remarkably upgraded by the irritation of LPS. Localization of Elrg in HepG2 cells was positioned mainly in cytoplasm. HepG2 cells were markedly arrested in the G1 phase by over-expressing Elrg. The percentage of HepG2 cells in G1 phase partly decreased after Elrg-siRNA. In conclusion, Elrg is probably correlative with LPS responding. Elrg is probably a new protein in cytoplasm which plays an important rolein regulating cell cycle. The results will deepen our understanding about the potential effects of Elrg on the human hepatoma-derived cell line HepG2.

机译：脂多糖（LPS）是革兰氏阴性细菌感染的毒性决定因素。 LPS的个体反应与其基因背景有关。有必要确定有关LPS的新分子和信号转导途径。进行本研究以评估新型环境脂多糖响应（Elrg）基因对肝癌衍生细胞系HepG2增殖和细胞周期调控的影响。通过RT-PCR，从人牙髓细胞cDNA文库中产生了新的Elrg分子。 LPS刺激显着提高了HepG2细胞中Elrg的表达水平。 Elrg在HepG2细胞中的定位主要位于细胞质中。通过过度表达Elrg，HepG2细胞明显停滞在G1期。 Elrg-siRNA后，G1期的HepG2细胞百分比部分降低。总之，Elrg可能与LPS反应相关。 Elrg可能是细胞质中的一种新蛋白，在调节细胞周期中起着重要作用。该结果将加深我们对Elrg对人肝癌衍生细胞HepG2的潜在作用的了解。

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来源
《Toxicology: An International Journal Concerned with the Effects of Chemicals on Living Systems》 |2008年第3期|共8页
作者
Du K; Chai Y; Hou L; Chang W; Chen S; Luo W; Cai T; Zhang X; Chen N; Chen Y; Chen J;
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正文语种 eng
中图分类毒物学（毒理学）;
关键词
Lipopolysaccharides; Human; Primary carcinoma of the liver cells; Genes; 脂多糖类; 基因; 细胞系;

机译：Lipopolysaccharides;Human;Primary carcinoma of the liver cells;Genes;脂多糖类;基因;细胞系;

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1. Over-expression and siRNA of a novel environmental lipopolysaccharide-responding gene on the cell cycle of the human hepatoma-derived cell line HepG2. [J] . Du K, Chai Y, Hou L, Toxicology: An International Journal Concerned with the Effects of Chemicals on Living Systems . 2008,第3期

机译：一个新的环境脂多糖响应基因在人肝癌衍生细胞系HepG2的细胞周期中的过表达和siRNA。
2. The effects of cyclooxygenase-2 gene silencing by siRNA on cell proliferation, cell apoptosis, cell cycle and tumorigenicity of Capan-2 human pancreatic cancer cells [J] . ZhongY., XiaZ., LiuJ., Oncology reports . 2012,第4期

机译：siRNA沉默环氧合酶-2基因对人胰腺癌Capan-2细胞增殖，细胞凋亡，细胞周期和致瘤性的影响
3. 1,25-Dihydroxyvitamin D(3) induced cell cycle arrest in the human primary liver cancer cell line HepG2. [J] . Morris DL Hepatology research: the official journal of the Japan Society of Hepatology . 2003,第1期

机译：1,25-Dihydroxyvitamin D（3）在人类原发性肝癌细胞HepG2中诱导细胞周期停滞。
4. Gene expression inhibition of N-Myc downregulated gene 1 (NDRG1) monitoring and facilitation via transfectional transfer of NDRG1-siRNA constructs into- in vitro-cultured human glioblastoma cells [C] . Said Harun M., Polat Buelent, Guckenberger Mathias, 2011 4th International Conference on Biomedical Engineering and Informatics . 2011

机译：通过将NDRG1-siRNA构建体转染至体外培养的人成胶质细胞瘤细胞中，N-Myc基因下调的基因1（NDRG1）的监测和促进基因表达抑制
5. DNA mismatch repair at an oncogene hotspot correlated with phase of the cell cycle and environmentally relevant concentrations of the Arctic pollutant p,p'-DDE. [D] . Simonetti, Josephine Patricia. 2001

机译：在癌基因热点的DNA错配修复与细胞周期的阶段和北极污染物p，p'-DDE的环境相关浓度有关。
6. Complement biosynthesis by the human hepatoma-derived cell line HepG2. [O] . K M Morris, D P Aden, B B Knowles, 1982

机译：补充人肝癌衍生细胞系HepG2的生物合成。
7. Complement biosynthesis by the human hepatoma-derived cell line HepG2. [O] . Morris, K M, Aden, D P, Knowles, B B, 1982

机译：补充人肝癌衍生细胞系HepG2的生物合成。

Over-expression and siRNA of a novel environmental lipopolysaccharide-responding gene on the cell cycle of the human hepatoma-derived cell line HepG2.

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