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[苯并(a)芘和佛波酯转化细胞系的建立及其生物学特性]

[The establishment of B(a)P and TPA transformed cell line and its biological characteristics].

作者信息

Pan Hong-ya, Zhang Zhi-yuan, Zhou Xiao-jian, Li Jiang, Zhang Ping, Chen Wan-tao

机构信息

Department of Oral and Maxillofacial Surgery, School of Stomatology, Shanghai Key Lab of Stomatology, Ninth People's Hospital, School of Medicine, Shanghai Jiao Tong University, Shanghai 200011, China.

出版信息

Shanghai Kou Qiang Yi Xue. 2006 Apr;15(2):152-6.

Abstract

PURPOSES

To transform HPV E6/E7 immortalized human oral epithelial cell line HIOEC cells by benzo(a)pyrene B(a)P and tetradecanoyl phorbol acetate (TPA) in vitro, and establish a carcinogenesis model of oral squamous cell carcinoma.

METHODS

HIOEC cells were treated with 0.1 microg/ml -1.2 microg/ml B(a)P for 6 months. Some of these cells were treated with 0.1 microg/ml TPA 24 hours at 4th passage and 10th passage, respectively. The cells were cloned at 18th passage, and then were cultured with DMEM medium contain 10% FBS at 21st passage. The cells were cultured in vitro for 1 year and developed into a malignant cell line HIOEC-B(a)P-TPA. The morphological changes of the cells were observed with differential interference contrast microscope and HE staining. The expression of cytokeratin and vimentin was identified with immunohistochemical staining. The soft agar colonies forming ability and tumorigenesity of the cells were identified to confirm the malignant characteristics of HIOEC-B(a)P-TPA cells.

RESULTS

(1) After HIOEC cells were treated with B(a)P plus TPA for 6 months, HIOEC-B(a)P-TPA cells grew well in DMEM medium containing with physical concentration of calcium and 10% FBS. (2) During HIOEC cells were treated with chemical carcinogens, the morphology of the cells was changed. HIOEC-B(a)P-TPA cells showed as fibroblast-like cells with many atypical mitosis. (3) The expression of cytokeratin decreased in the cells while that of vimentin increased in the cells. (4) HIOEC-B(a)P-TPA cells had strong soft agar colony formation ability and the colony formation ratio was 24.5%. (5) HIOEC-B(a)P-TPA cells have no tumorigenisity till now.

CONCLUSIONS

We established a biological factors and chemical carcinogens induced malignant cell line-HIOEC-B(a)P-TPA after a long period. It will provide a good multiple factors, multistage carcinogenesis model of OSCC for further research.

摘要

目的

体外通过苯并(a)芘(B(a)P)和十四酰佛波醇乙酸酯(TPA)转化人乳头瘤病毒E6/E7永生化人口腔上皮细胞系HIOEC细胞,建立口腔鳞状细胞癌的致癌模型。

方法

用0.1μg/ml - 1.2μg/ml的B(a)P处理HIOEC细胞6个月。其中部分细胞分别在第4代和第10代时用0.1μg/ml TPA处理24小时。在第18代时对细胞进行克隆,然后在第21代时用含10%胎牛血清的DMEM培养基培养。将细胞体外培养1年,形成恶性细胞系HIOEC-B(a)P-TPA。用微分干涉相差显微镜和苏木精-伊红染色观察细胞的形态变化。用免疫组织化学染色鉴定细胞角蛋白和波形蛋白的表达。鉴定细胞的软琼脂集落形成能力和致瘤性,以确认HIOEC-B(a)P-TPA细胞的恶性特征。

结果

(1) HIOEC细胞经B(a)P加TPA处理6个月后,HIOEC-B(a)P-TPA细胞在含生理浓度钙和10%胎牛血清的DMEM培养基中生长良好。(2) 在HIOEC细胞用化学致癌物处理期间,细胞形态发生改变。HIOEC-B(a)P-TPA细胞表现为成纤维细胞样细胞,有许多非典型有丝分裂。(3) 细胞中细胞角蛋白表达降低,而波形蛋白表达增加。(4) HIOEC-B(a)P-TPA细胞具有很强的软琼脂集落形成能力,集落形成率为24.5%。(5) 目前HIOEC-B(a)P-TPA细胞无致瘤性。

结论

经过长期培养,我们建立了一种生物因素和化学致癌物诱导的恶性细胞系 - HIOEC-B(a)P-TPA。它将为进一步研究提供一个良好的口腔鳞状细胞癌多因素、多阶段致癌模型。

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