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Regulation of differentiation- and proliferation-inducers on Lewis antigens α-fucosyltransferase and metastaticotential in hepatocarcinoma cells

机译：分化和增殖诱导物对肝癌细胞Lewis抗原α-岩藻糖基转移酶和转移势的调节

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The expressions of Lewis (Le) antigens, α-1,3/1,4 fucosyltransferases (α-1,3/1,4 FuTs), and metastatic potential after the treatment of 2 differentiation inducers, all- trans retinoic acid (ATRA), 8-bromo-cyclic 3′,5′adenosine monophosphate (8-Br-cAMP); and 2 proliferation inducers, epidermal growth factor (EGF) and phobol-12-myristate-13-acetate (PMA), on 7721 human hepatocarcinoma cell line were studied. Cell adhesion to human umbilical vein endothelial cells (HUVEC), cell migration through transwell and invasion through matrigel were selected as the indexes of metastatic potential-related phenotypes. Using fluorescence-labelled antibodies and flow-cytometric analysis, it was found that 7721 cells mainly expressed sialyl Lewis X (SLe^x) and a less amount of sialyl dimeric Lewis X (SDLe^x) antigens on the cell surface. Their expressions were down-regulated by ATRA, and up-regulated by EGF. SLe^xantigen was also decreased and increased by the treatment of 8-Br-cAMP and PMA respectively. With Northern blot to detect the mRNAs of α-1,3/1,4 FuTs, the main enzymatic basis for the change in SLe^xexpression was found to be the alteration of the expression of α-1,3 FuT-VII. It was evidenced by the observations that α-1,3 FuT-VII was the main α-1,3/1,4 FuT in 7721 cells, while α-1,3/1,4 FuT-III and α-1,3 FuT-VI were expressed rather low. The changes in the expressions of SLe^xantigen and α-1,3 FuT-VII resulted in the altered cell adhesion to tumour necrosis factor-α stimulated HUVEC, since only the monoclonal antibody of the SLe^x, but not other monoclonal antibodies blocked the adhesion of 7721 cells to HUVEC. The migration and invasion of 7721 cells were also reduced by the treatment of ATRA or 8-Br-cAMP, and elevated by EGF or PMA. The above findings indicate that the metastatic potential of 7721 cells is suppressed by differentiation-inducers and promoted by proliferation-inducers. © 2001 Cancer Research Campaign

机译：两种分化诱导剂全反式维甲酸（ATRA）处理后，Lewis（Le）抗原α-1,3/ 1,4岩藻糖基转移酶（α-1,3/ 1,4 FuTs）的表达和转移潜能），8-溴环3'，5'腺苷一磷酸（8-Br-cAMP）;研究了7721种人肝癌细胞系中的2种增殖诱导剂，表皮生长因子（EGF）和phobol-12-肉豆蔻酸酯-13-乙酸酯（PMA）。选择与人脐静脉内皮细胞（HUVEC）粘附的细胞，通过穿孔的细胞迁移和通过基质胶侵袭的细胞作为转移潜能相关表型的指标。使用荧光标记的抗体和流式细胞仪分析，发现7721细胞主要表达唾液酸化的Lewis X（SLe ^{x ）和较少量的唾液酸二聚体的Lewis X（SDLe ^{x ）细胞表面的抗原。它们的表达被ATRA下调，并被EGF上调。 SBr ^{x 抗原也分别通过8-Br-cAMP和PMA处理而降低和增加。用Northern印迹检测α-1,3/ 1,4 FuTs的mRNA，发现SLe ^{x 表达变化的主要酶学基础是α-1表达的改变。，3 FuT-VII。观察结果表明，α-1,3FuT-VII是7721细胞中主要的α-1,3/ 1,4 FuT，而α-1,3/ 1,4 FuT-III和α-1， 3 FuT-VI的表达水平较低。 SLe ^{x 抗原和α-1,3FuT-VII的表达变化导致细胞对肿瘤坏死因子-α刺激的HUVEC的粘附性改变，因为仅SLe ^{x ，但没有其他单克隆抗体阻止7721细胞与HUVEC的粘附。通过处理ATRA或8-Br-cAMP也可以减少7721细胞的迁移和侵袭，而通过EGF或PMA可以提高其迁移和侵袭。上述发现表明，分化诱导剂抑制了7721细胞的转移潜能，而增殖诱导剂则促进了其转移潜能。 ©2001癌症研究运动}}}}}}

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期刊名称 British Journal of Cancer
作者
F Liu; H-L Qi; H-L Chen;
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年(卷),期 2001(84),11
年度 2001
页码 1556–1563
总页数 8
原文格式 PDF
正文语种
中图分类肿瘤学;
关键词
human hepatocarcinoma cells differentiation-inducer proliferation-inducer Lewis antigen α-fucosyltransferase metastasis-related phenotype;

机译：人肝癌细胞;分化诱导剂;增殖诱导剂;Lewis抗原;α-岩藻糖基转移酶;与转移相关的表型;

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专利

1. Regulation of differentiation- and proliferation-inducers on Lewis antigens, |[alpha]|-fucosyltransferase and metastaticpotential in hepatocarcinoma cells [J] . British Journal of Cancer . 2001,第11期

机译：肝癌细胞中Lewis抗原，|α|-岩藻糖基转移酶和转移潜能的分化和增殖诱导剂的调控
2. Analysis of lewis antigens on cell surface and alpha1,3 fucosyltransferase subtypes in H7721 human hepatocarcinoma cells. [J] . Guo P, Zhang Y, Zhang XY, Journal of experimental & clinical cancer research : . 2003,第1期

机译：H7721人肝癌细胞中细胞表面的刘易斯抗原和alpha1,3岩藻糖基转移酶亚型的分析。
3. Transfection of the nm23-H1 gene into human hepatocarcinoma cell line inhibits the expression of sialyl Lewis X, alpha1,3 fucosyltransferase VII, and metastatic potential. [J] . Liu F, Zhang Y, Zhang XY, Journal of Cancer Research and Clinical Oncology . 2002,第4期

机译：将nm23-H1基因转染到人肝癌细胞系中会抑制唾液酸化Lewis X，α1,3岩藻糖基转移酶VII的表达和转移潜能。
4. Synthesis of glycopeptides with Lewis antigen or sialyl-Lewis~x antigen side chains [C] . Horst Kunz, Karsten von dem Bruch, G.Kretzschmar, Chinese peptide symposium . 1998

机译：用Lewis抗原或SiaLyl-Lewis〜X抗原侧链合成糖肽
5. Regulation of adaptive immune responses by the phagocyte-type NADPH oxidase in T cells and antigen presenting cells [D] . Shatynski, Kristen Elizabeth 2012

机译：T细胞和抗原呈递细胞中吞噬细胞型NADPH氧化酶对适应性免疫应答的调节
6. Towards abolition of immunogenic structures in insect cells: characterization of a honey-bee (Apis mellifera) multi-gene family reveals both an allergy-related core α13-fucosyltransferase and the first insect Lewis-histo-blood-group-related antigen-synthesizing enzyme [O] . Dubravko Rendić, Jaroslav Klaudiny, Ute Stemmer, 2007

机译：努力消除昆虫细胞中的免疫原性结构：对蜜蜂（Apis mellifera）多基因家族进行鉴定揭示了与过敏相关的核心α13-岩藻糖基转移酶和第一个与昆虫Lewis-组织-血型相关的抗原-合成酶
7. Regulation of differentiation- and proliferation-inducers on Lewis antigens, α-fucosyltransferase and metastaticotential in hepatocarcinoma cells [O] . Liu, F, Qi, H-L, Chen, H-L 2001

机译：分化和增殖诱导物对肝癌细胞Lewis抗原，α-岩藻糖基转移酶和转移势的调节
8. Reactivity of Lewis Lymph Node and Bone Marrow Cells to F344 Non-AgB Histocompatibility Antigens [R] . Schlagel, C. J., Lubaroff, D. M. 1979

机译：Lewis淋巴结和骨髓细胞对F344非agB组织相容性抗原的反应性

Regulation of differentiation- and proliferation-inducers on Lewis antigens α-fucosyltransferase and metastaticotential in hepatocarcinoma cells

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