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首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >Study of immortalization and malignant transformation of human embryonic esophageal epithelial cells induced by HPV18 E6E7
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Study of immortalization and malignant transformation of human embryonic esophageal epithelial cells induced by HPV18 E6E7

机译:HPV18 E6E7诱导人胚食管上皮细胞永生化和恶性转化的研究

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In order to study the effect of viruses and tumor promoters on the tumorigenicity of the esophagus, human embryonic esophageal epithelial cells were infected with human papilloma virus HPV18 E6E7-AAV in synergy with 12-O-tetradecanoylphorboll.3-acetate (TPA) to observe their malignant transformation. The cultured esophageal epithelial cells incubated with HPV18 E6E7-AAV were divided into two groups: the SHEEC1 group was exposed to TPA (5 ng/ml) for 4 weeks at the 5th passage of the cells; the SHEE group served as the control and was cultured in the same medium without TPA. The morphological phenotype, the DNA content during the cell cycle and the chromosomes were analyzed. The tumorigenicity was assessed by colony formation after cultivation in soft agar and transplanting the cells into nude mice. HPV18 E6E7 DNA was assayed by fluorescent in situ hybridization (FISH) and the polymerase chain reaction (PCR). The SHEE group, at its 20th passage, grew as a monolayer with the cells showing anchorage dependence and contact inhibition. The chromosome analysis showed diploidy, and soft-agar cultivation and injection into nude mice showed the cells to be non-tumorigenic. They were therefore immortalized cells. In contrast, the SHEEC1 group (TPA group) showed increased DNA synthesis and a proliferative index that was higher (45%) than that of the SHEE group (34%). The number of large colonies of dense multilayer cells (positively transformed foci) in soft agar was high in SHEEC1 group (4.0%) but low in the SHEE group (0.1%). Tumors resulting from transplantation were observed in all six nude mice injected subcutaneously with cells of the SHEEC1 group but no tumor developed in mice receiving cells of the SHEE group. In both groups of cells, HPV18 E6E7 DNA was positively detected by FISH and PCR. The malignant transformation of human embryonic epithelial cells was induced in vitro by HPV18 E6E7 in synergy with TPA. This is a good evidence for the close relationship between HPV and the etiology and pathoge-nicity of esophageal carcinoma. It is also a reliable model for studying the cellular and molecular mechanisms of carcinogenesis of esophageal carcinoma.
机译:为了研究病毒和肿瘤启动子对食道致瘤性的影响,将人乳头瘤病毒HPV18 E6E7-AAV与12-O-十四烷酰佛手脂3-乙酸盐(TPA)协同感染人胚胎食道上皮细胞,观察他们的恶变。将用HPV18 E6E7-AAV培养的食管上皮细胞分为两组:在第5次传代时,将SHEEC1组暴露于TPA(5 ng / ml)4周。 SHEE组作为对照,在没有TPA的相同培养基中培养。分析了细胞的形态表型,细胞周期内的DNA含量和染色体。通过在软琼脂中培养并将细胞移植到裸鼠中后的菌落形成来评估致瘤性。通过荧光原位杂交(FISH)和聚合酶链反应(PCR)测定HPV18 E6E7 DNA。 SHEE组在第20代以单层生长,其细胞表现出锚定依赖性和接触抑制作用。染色体分析显示为二倍体,软琼脂培养和裸鼠注射显示细胞为非致瘤细胞。因此,它们是永生的细胞。相反,SHEEC1组(TPA组)的DNA合成增加,其增殖指数(45%)高于SHEE组(34%)。在软琼脂中,密集的多层细胞(阳性转化的病灶)的大集落数在SHEEC1组中较高(4.0%),而在SHEE组中较低(0.1%)。在皮下注射了SHEEC1组细胞的所有六只裸鼠中均观察到了移植产生的肿瘤,但在接受SHEE组细胞的小鼠中未发现肿瘤。在两组细胞中,通过FISH和PCR阳性检测到HPV18 E6E7 DNA。 HPV18 E6E7与TPA协同在体外诱导人胚胎上皮细胞的恶性转化。这是HPV与食管癌的病因和病理学之间密切关系的良好证据。它也是研究食管癌致癌作用的细胞和分子机制的可靠模型。

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