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Characterization of telomerase-immortalized, non-neoplastic, human Barrett’s cell line (BAR-T)

端粒酶逆转录酶 端粒酶 细胞培养 癌症研究 肿瘤转化 化生 生物 恶性转化 病理 巴雷特食管 上皮 发育不良 分子生物学 腺癌 癌变 医学 癌症 遗传学 基因
作者
Kshama Jaiswal,Carmela P. Morales,Linda A. Feagins,Kenia Gandia,X. Zhang,H.-Y. Zhang,Kadija‐Kathy Hormi‐Carver,Yuenan Shen,F.F.B. Elder,Ruben D. Ramirez,George A. Sarosi,Stuart J. Spechler,Rhonda F. Souza
出处
期刊:Diseases of The Esophagus [Oxford University Press]
卷期号:20 (3): 256-264 被引量:83
标识
DOI:10.1111/j.1442-2050.2007.00683.x
摘要

Barrett's esophagus, a metaplasia predisposed to malignant transformation, has been studied in vitro using esophageal adenocarcinoma cell lines. However, findings in such transformed cells may not be applicable to the non-neoplastic cells of benign Barrett's esophagus. Therefore, we have developed and characterized a Barrett's cell line derived from a patient without malignancy or dysplasia. Human Barrett's epithelial cells were immortalized with the insertion of hTERT (human telomerase reverse transcriptase) using a Cre-lox recombination system. We then examined properties of this continuous cell line, such as in vitro tumorigenicity, growth patterns, histological differentiation characteristics, karyotype, and checkpoint arrest mechanisms (e.g., p16, p21, and p53). Non-neoplastic Barrett's epithelial cells infected with hTERT (BAR-T cells) have been sustained in culture beyond 200 population doublings. BAR-T cells maintain a diploid chromosome number and exhibit non-neoplastic properties, such as contact inhibition and anchorage-dependent growth. BAR-T cells express differentiation Barrett's epithelial markers, such as villin and cytokeratins 4, 8 and 18, and stain positive for Alcian blue, indicating the presence of mucin-producing cells. Expression of checkpoint arrest proteins p21 and p53 are intact, while p16 expression is lost. Thus, we have created a human Barrett's cell line that is not malignantly transformed, and yet can be maintained indefinitely in culture. BAR-T cells are diploid, have histological differentiation markers characteristic of benign Barrett's epithelium, and also maintain appropriate expression of p21 and p53. This cell line should be a useful model for the study of the early events in carcinogenesis in Barrett's esophagus.

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