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首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >Establishment and long-term xenografting of human pancreatic carcinomas in immunosuppressed mice: changes and stability in morphology, DNA ploidy and proliferation activity.
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Establishment and long-term xenografting of human pancreatic carcinomas in immunosuppressed mice: changes and stability in morphology, DNA ploidy and proliferation activity.

机译:在免疫抑制小鼠中建立人胰腺癌并进行长期异种移植:形态,DNA倍性和增殖活性的变化和稳定性。

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The prognosis of pancreatic carcinoma is grave, therefore the experimental model systems remain major tools for testing new treatment modalities. We have developed human pancreatic cancer lines growing in immunosuppressed mice and characterized them by morphological and flow-cytometric studies. Immunosuppression has been achieved in young (4-week-old) CBA/CA mice by thymectomy, whole-body irradiation and bone marrow reconstruction. Twelve surgically removed human pancreatic carcinomas were implanted subcutaneously and serially transplantable xenografts have been established. Altogether 129 samples derived from 59 generations have been analyzed. Out of 12 carcinomas, 6 developed continuously growing and transplantable xenografts (PZX-2, PZX-5, PZX-11, PZX-15, PZX-16, PZX-20; take rate: 50%). They were successfully maintained for 9-16 passages, for 18-25 months. New subpopulations developed during transplantations in 3 tumor lines and these morphological changes have been reflected by the appearance of an aneuploid peak in flow cytometry. In 1 tumor line, however, DNA aneuploidy was observable despite the unaltered histology. The PZX-20 line retained its original morphology and aneuploid pattern during 9 consecutive passages and over 18 months. The results indicate that the artificially immunosuppressed CBA/CA mice are suitable hosts for accepting and maintaining human pancreatic carcinomas. During successive xenograftings the regular morphological characterization must be supplemented by flow cytometry, because new tumorous clones may develop despite the unchanged histological picture.
机译:胰腺癌的预后很严重,因此实验模型系统仍然是测试新治疗方式的主要工具。我们已经开发了在免疫抑制小鼠中生长的人类胰腺癌细胞,并通过形态学和流式细胞术研究对其进行了表征。通过胸腺切除术,全身照射和骨髓重建,已在年轻(4周龄)CBA / CA小鼠中实现了免疫抑制。皮下植入十二种通过手术切除的人类胰腺癌,并且已经建立了可系列移植的异种移植物。总共分析了59个世代中的129个样本。在12例癌症中,有6例发展为持续生长和可移植的异种移植物(PZX-2,PZX-5,PZX-11,PZX-15,PZX-16,PZX-20;摄取率:50%)。他们成功地维持了9-16代,持续了18-25个月。在3个肿瘤细胞系的移植过程中产生了新的亚群,这些形态变化已通过流式细胞仪中非整倍体峰的出现反映出来。然而,在1个肿瘤细胞系中,尽管组织学未改变,但仍可观察到DNA非整倍性。 PZX-20系列在连续9个传代过程中和超过18个月的时间内保持了其原始形态和非整倍体模式。结果表明,人工免疫抑制的CBA / CA小鼠是接受和维持人胰腺癌的合适宿主。在连续的异种移植过程中,必须通过流式细胞术来补充常规的形态学特征,因为尽管组织学图像不变,但仍可能形成新的肿瘤克隆。

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