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角质形成细胞生长因子可诱导转基因小鼠发生乳腺和前列腺增生以及乳腺腺癌。

Keratinocyte growth factor induces mammary and prostatic hyperplasia and mammary adenocarcinoma in transgenic mice.

作者信息

Kitsberg D I, Leder P

机构信息

Department of Genetics, Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

Oncogene. 1996 Dec 19;13(12):2507-15.

PMID:9000125
Abstract

The kinetics of solitary mammary tumor formation in transgenic mice bearing the MMTV-int-2 (fgf3) fusion gene suggest that several genetic events are required for tumorigenesis. In an effort to identify elements that could contribute to this oncogenic process, we used differential display PCR to identify gene products that are strongly and specifically induced in int-2 mammary tumors. Using this approach we identified a member of the FGF family, kgf (fgf7), as a gene that is strongly upregulated in an int-2-containing mammary tumor. Since int-2 and kgf strongly bind the same receptor, the IIIb isoform of FGFR2, it is possible that their joint expression, one as a transgene, the other as an activated gene, might reinforce the same mitogenic pathway. To test this possibility, we created transgenic mice that carry kgf as a transgene gene under the control of the MMTV promoter/enhancer. Female mice carrying this transgene develop a very dramatic mammary epithelial hyperplasia and go on to develop solitary, metastatic adenocarcinomas of the mammary gland. Consistent with a common signalling pathway, the MMTV-kgf-induced hyperplasia has the morphologic characteristics of that seen in the MMTV-int-2 mice. Male mice also develop hyperplasia of the male genital tract, including the seminal vesicle, the vas deferens and the prostate. Thus KGF can act as a potent proliferative inducer in mammary and specific urogenital tissue and can contribute to the development of adenocarcinoma of the mammary gland in a manner strongly reminiscent of receptor-related ligand, int-2.

摘要

携带MMTV-int-2(fgf3)融合基因的转基因小鼠中孤立性乳腺肿瘤形成的动力学表明,肿瘤发生需要多个遗传事件。为了确定可能促成这一致癌过程的因素,我们使用差异显示PCR来鉴定在int-2乳腺肿瘤中强烈且特异性诱导的基因产物。通过这种方法,我们鉴定出FGF家族的一个成员kgf(fgf7),它是在含int-2的乳腺肿瘤中强烈上调的基因。由于int-2和kgf强烈结合相同的受体,即FGFR2的IIIb同种型,它们的联合表达,一个作为转基因,另一个作为激活基因,可能会加强相同的促有丝分裂途径。为了验证这种可能性,我们创建了在MMTV启动子/增强子控制下携带kgf作为转基因的转基因小鼠。携带这种转基因的雌性小鼠会发生非常显著的乳腺上皮增生,并继而发展为孤立性、转移性乳腺腺癌。与共同的信号通路一致,MMTV-kgf诱导的增生具有在MMTV-int-2小鼠中所见的形态学特征。雄性小鼠也会发生雄性生殖道增生,包括精囊、输精管和前列腺。因此,KGF可作为乳腺和特定泌尿生殖组织中的强效增殖诱导剂,并能以强烈类似于受体相关配体int-2的方式促成乳腺腺癌的发展。

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