小鼠乳腺肿瘤病毒c-rel转基因小鼠会发生乳腺肿瘤。
Mouse mammary tumor virus c-rel transgenic mice develop mammary tumors.
作者信息
Romieu-Mourez Raphaëlle, Kim Dong W, Shin Sang Min, Demicco Elizabeth G, Landesman-Bollag Esther, Seldin David C, Cardiff Robert D, Sonenshein Gail E
机构信息
Department of Biochemistry, Boston University Medical School, Boston, Massachusetts 02118, USA.
出版信息
Mol Cell Biol. 2003 Aug;23(16):5738-54. doi: 10.1128/MCB.23.16.5738-5754.2003.
Amplification, overexpression, or rearrangement of the c-rel gene, encoding the c-Rel NF-kappaB subunit, has been reported in solid and hematopoietic malignancies. For example, many primary human breast cancer tissue samples express high levels of nuclear c-Rel. While the Rev-T oncogene v-rel causes tumors in birds, the ability of c-Rel to transform in vivo has not been demonstrated. To directly test the role of c-Rel in breast tumorigenesis, mice were generated in which overexpression of mouse c-rel cDNA was driven by the hormone-responsive mouse mammary tumor virus long terminal repeat (MMTV-LTR) promoter, and four founder lines identified. In the first cycle of pregnancy, the expression of transgenic c-rel mRNA was observed, and levels of c-Rel protein were increased in the mammary gland. Importantly, 31.6% of mice developed one or more mammary tumors at an average age of 19.9 months. Mammary tumors were of diverse histology and expressed increased levels of nuclear NF-kappaB. Analysis of the composition of NF-kappaB complexes in the tumors revealed aberrant nuclear expression of multiple subunits, including c-Rel, p50, p52, RelA, RelB, and the Bcl-3 protein, as observed previously in human primary breast cancers. Expression of the cancer-related NF-kappaB target genes cyclin D1, c-myc, and bcl-xl was significantly increased in grossly normal transgenic mammary glands starting the first cycle of pregnancy and increased further in mammary carcinomas compared to mammary glands from wild-type mice or virgin transgenic mice. In transient transfection analysis in untransformed breast epithelial cells, c-Rel-p52 or -p50 heterodimers either potently or modestly induced cyclin D1 promoter activity, respectively. Lastly, stable overexpression of c-Rel resulted in increased cyclin D1 and NF-kappaB p52 and p50 subunit protein levels. These results indicate for the first time that dysregulated expression of c-Rel, as observed in breast cancers, is capable of contributing to mammary tumorigenesis.
编码c-Rel核因子-κB亚基的c-rel基因的扩增、过表达或重排已在实体瘤和血液系统恶性肿瘤中被报道。例如,许多原发性人类乳腺癌组织样本表达高水平的核c-Rel。虽然Rev-T癌基因v-rel可在鸟类中引发肿瘤,但c-Rel在体内的转化能力尚未得到证实。为了直接测试c-Rel在乳腺肿瘤发生中的作用,构建了小鼠模型,其中小鼠c-rel cDNA的过表达由激素反应性小鼠乳腺肿瘤病毒长末端重复序列(MMTV-LTR)启动子驱动,并鉴定出四个奠基系。在第一个妊娠周期中,观察到转基因c-rel mRNA的表达,且乳腺中c-Rel蛋白水平升高。重要的是,31.6%的小鼠在平均19.9个月龄时发生了一个或多个乳腺肿瘤。乳腺肿瘤具有多种组织学类型,并表达升高水平的核因子-κB。对肿瘤中核因子-κB复合物组成的分析显示多个亚基的异常核表达,包括c-Rel、p50、p52、RelA、RelB和Bcl-3蛋白,这与先前在人类原发性乳腺癌中观察到的情况一致。从第一个妊娠周期开始,在大体正常的转基因乳腺中,癌症相关的核因子-κB靶基因细胞周期蛋白D1、c-myc和bcl-xl的表达显著增加,与野生型小鼠或未生育转基因小鼠相比,在乳腺癌中进一步增加。在未转化的乳腺上皮细胞的瞬时转染分析中,c-Rel-p52或-p50异二聚体分别强力或适度诱导细胞周期蛋白D1启动子活性。最后,c-Rel的稳定过表达导致细胞周期蛋白D1以及核因子-κB p52和p50亚基蛋白水平升高。这些结果首次表明,如在乳腺癌中观察到的,c-Rel的表达失调能够促进乳腺肿瘤发生。
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