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Development of PIN and Prostate Adenocarcinoma Cell Lines: A Model System for Multistage Tumor Progression1

机译:PIN和前列腺腺癌细胞系的开发:多阶段肿瘤进展的模型系统1

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摘要

Existing prostate cancer cell lines have been derived from late stages of human prostate cancer. In this paper, we present two cell lines generated from prostatic intraepithelial neoplasia (PIN), the precursor lesion for prostate adenocarcinoma. Pr-111 and Pr-117 were established from PIN lesions that developed in the C3(1)/Tag transgenic model of prostate cancer. Pr-111 and Pr-117 cells express simian virus 40 large T antigen (SV40 Tag) and are immortalized in culture, distinguishing them from normal prostate cells. The growth rates of these two cell lines are quite different; with Pr-111 cells growing much more slowly (doubling time approximately 40 hours) compared to Pr-117 cells (doubling time approximately 22 hours), and also show significantly different growth rates in different media. Both prostate cell lines express cytokeratin and androgen receptor (AR) with Pr-111 cells demonstrating androgen-dependent growth and Pr-117 cells exhibiting androgen-responsive growth characteristics. Athymic nude mice injected with Pr-111 cells either do not develop tumors or develop tumors after a long latency period of 14 weeks. Pr-117 cells, however, develop tumors by 3 to 6 weeks, suggesting that Pr-117 cells represent a later stage of tumor progression. These two novel cell lines will be useful for studying early stages of prostate tumor development and androgen responsiveness.
机译:现有的前列腺癌细胞系已经衍生自人类前列腺癌的晚期。在本文中,我们介绍了两种由前列腺上皮内瘤变(PIN)(前列腺腺癌的前体病变)产生的细胞系。 Pr-111和Pr-117是从在前列腺癌的C3(1)/ Tag转基因模型中发展的PIN病变建立的。 Pr-111和Pr-117细胞表达猿猴病毒40大T抗原(SV40标签),并在培养中永生化,从而将它们与正常前列腺细胞区分开。这两种细胞系的生长率差异很大。 Pr-111细胞的生长速度(倍增时间约40小时)比Pr-117细胞的生长速度(倍增时间约22小时)要快得多,并且在不同培养基中的生长速度也明显不同。两种前列腺细胞系均表达细胞角蛋白和雄激素受体(AR),其中Pr-111细胞表现出雄激素依赖性生长,而Pr-117细胞表现出雄激素响应性生长特征。注射Pr-111细胞的无胸腺裸鼠在经过14周的长时间潜伏期后未出现肿瘤或未出现肿瘤。但是,Pr-117细胞会在3至6周内发展成肿瘤,这表明Pr-117细胞代表了肿瘤进展的后期。这两种新的细胞系将有助于研究前列腺肿瘤发展和雄激素反应的早期阶段。

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