首页> 外文期刊>Japanese Journal of Cancer Research >Selective inhibition of hepatoma cells using diphtheria toxin A under the control of the promoter/enhancer region of the human alpha-fetoprotein gene.
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Selective inhibition of hepatoma cells using diphtheria toxin A under the control of the promoter/enhancer region of the human alpha-fetoprotein gene.

机译:在人α-甲胎蛋白基因的启动子/增强子区域的控制下,使用白喉毒素A选择性抑制肝癌细胞。

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摘要

We constructed a plasmid containing human alpha-fetoprotein (AFP) promoter/enhancer to direct the cell type-specific expression of diphtheria toxin fragment A (DTA), designated as pAF-DTA, to AFP-producing hepatocellular carcinoma cells. The transfection was carried out with cationic liposomes (DMRIE-C) and the expression of the DTA gene was confirmed by a northern blot analysis. When pAF-DTA was transfected, the growth of AFP-positive HuH-7 cells was inhibited, whereas growth inhibition was not observed in AFP-negative MKN45 cells. In this experiment, the secretion of AFP was similarly suppressed, but the secretion of carcinoembryonic antigen from MKN45 was not altered. pAF-DTA could also exert its growth inhibitory effect on PLC, a cell line with a low level of AFP. However, no inhibitory effect of pAF-DTA was observed on the proliferation of primary hepatocyte cells. Furthermore, transfection experiments in which HuH-7 and splenic stromal cells were co-cultured revealed the growth inhibition by pAF-DTA to be selective in HuH-7 cells. Finally, the growth of HuH-7 transplanted on BALB/c nuu mice was inhibited by the direct injection of pAF-DTA/liposome complex into a tumor mass. These results suggest that use of pAF-DTA may be potentially useful as a novel approach for the selective treatment of tumor cells producing AFP even at low levels, without affecting other types of cells.
机译:我们构建了一个包含人α甲胎蛋白(AFP)启动子/增强子的质粒,以将白喉毒素片段A(DTA)的细胞类型特异性表达(称为pAF-DTA)引导至产生AFP的肝癌细胞。用阳离子脂质体(DMRIE-C)进行转染,并通过RNA印迹分析确认DTA基因的表达。当转染pAF-DTA时,AFP阳性HuH-7细胞的生长受到抑制,而在AFP阴性的MKN45细胞中未观察到生长抑制。在该实验中,类似地抑制了AFP的分泌,但是来自MKN45的癌胚抗原的分泌没有改变。 pAF-DTA还可以对PLC(一种AFP水平较低的细胞系)发挥生长抑制作用。然而,未观察到pAF-DTA对原代肝细胞增殖的抑制作用。此外,HuH-7和脾基质细胞共培养的转染实验表明,pAF-DTA的生长抑制在HuH-7细胞中具有选择性。最后,通过将pAF-DTA /脂质体复合物直接注射到肿瘤块中来抑制移植到BALB / c nu / nu小鼠上的HuH-7的生长。这些结果表明,pAF-DTA的使用可能潜在地作为一种选择性治疗产生AFP的肿瘤细胞的新方法,即使在低水平下也不影响其他类型的细胞。

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