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Establishment and Characterization of Two Novel Human Pancreatic Carcinoma Cell Lines

机译:两种新型人胰腺癌细胞系的建立和表征

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Background: Pancreatic carcinoma (PC) is among the most lethal types of carcinomas worldwide. We aimed to establish well-defined PC cell lines in order to determine their resistance to chemotherapy. Materials and Methods: Cells cultured from the tumors of two patients were analyzed for xenograft formation, V-Ki-ras2 Kirsten rat sarcoma viral oncogene homolog (KRAS) and TP53 mutations, chemosensitivity, and mRNAs encoding rate-limiting enzymes that metabolize anticancer drugs. Results: The TYPK-1 and TYPK-2 cell lines were established from the lymph node of a locally advanced PC and from the ascites of a multi-metastatic and multi-chemoresistant PC, respectively. Each cell line generated tumors in nude mice. KRAS and TP53 mutations were detected in TYPK-1 but not TYPK-2 cells. TYPK-1 cells were resistant to gemcitabine, and TYPK-2 cells were resistant to oxaliplatin. The gemcitabine sensitivity of each cell line correlated with the expression of mRNAs encoding DCK and SLCAC29A1. Conclusion: TYPK-1 and TYPK-2 cells may contribute to investigations of resistance to anticancer drugs.
机译:背景:胰腺癌(PC)是世界上最致命的癌症之一。我们旨在建立定义明确的PC细胞系,以确定其对化学疗法的抗性。材料和方法:分析了两名患者肿瘤中培养的细胞的异种移植物形成,V-Ki-ras2 Kirsten大鼠肉瘤病毒癌基因同源物(KRAS)和TP53突变,化学敏感性以及编码可代谢抗癌药物的限速酶的mRNA。结果:TYPK-1和TYPK-2细胞系分别从局部晚期PC的淋巴结和多转移和多耐药PC的腹水建立。每个细胞系在裸鼠中均产生肿瘤。在TYPK-1细胞中检测到KRAS和TP53突变,而在TYPK-2细胞中未检测到。 TYPK-1细胞对吉西他滨有抗性,而TYPK-2细胞对奥沙利铂有抗性。每个细胞系的吉西他滨敏感性与编码DCK和SLCAC29A1的mRNA表达有关。结论:TYPK-1和TYPK-2细胞可能有助于抗癌药物的研究。

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