c-myc单转基因和tgf - α /c-myc双转基因小鼠的肝肿瘤诱导。

S S Thorgeirsson, E Santoni-Rugiu, C D Davis, E G Snyderwine
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引用次数: 8

摘要

我们培育了携带由小鼠白蛋白增强子/启动子-小鼠c-myc cDNA和小鼠金属硫蛋白1启动子-人tgf - α cDNA组成的融合基因的双转基因小鼠,以研究这些基因在肝癌发生过程中的相互作用,并为表征核癌基因和生长因子在肿瘤发生过程中的相互作用提供了一个通用范例,同时也建立了一个实验模型来测试环境化学物质在肝癌发生过程中如何与这些基因相互作用肿瘤形成过程。与单独表达这两种转基因中的任何一种相比,在小鼠肝脏中,作为转基因的c-myc和tgf - α的共表达导致该器官肿瘤发展的极大加速。在肝脏肿瘤出现之前,双转基因小鼠的肝脏中发生了两种不同的细胞反应,即现有肝细胞的发育不良和凋亡改变,随后出现由增生性和发育不良细胞群组成的多个局灶性病变。这些观察结果表明,在肝肿瘤的发展过程中,c-myc和tgf - α的相互作用有助于肿瘤前细胞群的选择和扩增,从而增加恶性转化的可能性。用二乙基亚硝胺和IQ等基因毒性药物以及肿瘤启动剂苯巴比妥治疗双转基因小鼠,大大加速了肿瘤的形成过程。这些结果表明,选择性转基因小鼠模型可能为测试环境化学物质的致癌潜力以及这些化合物在肿瘤形成过程中与特定基因的相互作用/合作提供重要工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Hepatic tumor induction in c-myc mono-transgenic and TGF-alpha/c-myc double-transgenic mice.

Double transgenic mice bearing fusion genes consisting of mouse albumin enhancer/promoter-mouse c-myc cDNA and mouse metallothionein 1 promoter-human TGF-alpha cDNA were generated to investigate the interaction of these genes in hepatic oncogenesis and to provide a general paradigm for characterizing both the interaction of nuclear oncogenes and growth factors in tumorigenesis as well as to produce an experimental model to test how environmental chemicals might interact with these genes during the neoplastic process. Coexpression of c-myc and TGF-alpha as transgenes in the mouse liver resulted in a tremendous acceleration of neoplastic development in this organ as compared to expression of either of these transgenes alone. The two distinct cellular reactions that occurred in the liver of the double transgenic mice prior to the appearance of liver tumors were dysplastic and apoptotic changes in the existing hepatocytes followed by emergence of multiple focal lesions composed of both hyperplastic and dysplastic cell populations. These observations suggest that the interaction of c-myc and TGF-alpha, during development of hepatic neoplasia contributes to the selection and expansion of the preneoplastic cell populations which consequently increases the probability of malignant conversion. Treatment of the double transgenic mice with both genotoxic agents such as diethylnitrosamine and IQ as well as the tumor promoter phenobarbital greatly accelerated the neoplastic process. These results suggest that selective transgenic mouse models may provide important tools for testing both the carcinogenic potential of environmental chemicals and the interaction/cooperation of these compounds with specific genes during the neoplastic process.

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