Knockout and transgenic mice of Trp53: What have we learned about p53 in breast cancer?

被引:16
作者
Blackburn A.C. [1 ]
Jerry D.J. [1 ]
机构
[1] Dept. of Veterinary/Animal Sciences, Paige Laboratory, University of Massachusetts, Amherst
来源
Breast Cancer Research | / 4卷 / 3期
关键词
Breast cancer; Knockout; p53; Transgenic;
D O I
10.1186/bcr427
中图分类号
学科分类号
摘要
The human p53 tumor suppressor gene TP53 is mutated at a high frequency in sporadic breast cancer, and Li-Fraumeni syndrome patients who carry germline mutations in one TP53 allele have a high incidence of breast cancer. In the 10 years since the first knockout of the mouse p53 tumor suppressor gene (designated Trp53) was published, much has been learned about the contribution of p53 to biology and tumor suppression in the breast through the use of p53 transgenic and knockout mice. The original mice deficient in p53 showed no mammary gland phenotype. However, studies using BALB/c-Trp53-deficient mice have demonstrated a delayed involution phenotype and a mammary tumor phenotype. Together with other studies of mutant p53 transgenes and p53 bitransgenics, a greater understanding has been gained of the role of p53 in involution, of the regulation of p53 activity by hormones, of the effect of mouse strain and modifier genes on tumor phenotype, and of the cooperation between p53 and other oncogenic pathways, chemical carcinogens and hormonal stimulation in mammary tumorigenesis. Both p53 transgenic and knockout mice are important in vivo tools for understanding breast cancer, and are yet to be exploited for developing therapeutic strategies in breast cancer.
引用
收藏
页码:101 / 111
页数:10
相关论文
共 65 条
[41]  
Hadsell D.L., Murphy K.L., Bonnette S.G., Reece N., Laucirica R., Rosen J.M., Cooperative interaction between mutant p53 and des(1-3)IGF-I accelerates mammary tumorigenesis, Oncogene, 19, pp. 889-898, (2000)
[42]  
Donehower L.A., Godley L.A., Aldaz C.M., Pyle R., Shi Y.P., Pinkel D., Gray J., Bradley A., Medina D., Varmus H.E., Deficiency of p53 accelerates mammary tumorigenesis in Wnt-1 transgenic mice and promotes chromosomal instability, Genes Dev, 9, pp. 882-895, (1995)
[43]  
Hundley J.E., Koester S.K., Troyer D.A., Hilsenbeck S.G., Subler M.A., Windle J.J., Increased tumor proliferation and genomic instability without decreased apoptosis in MMTV-ras mice deficient in p53, Mol. Cell Biol, 17, pp. 723-731, (1997)
[44]  
Jones J.M., Attardi L., Godley L.A., Laucirica R., Medina D., Jacks T., Varmus H.E., Donehower L.A., Absence of p53 in a mouse mammary tumor model promotes tumor cell proliferation without affecting apoptosis, Cell Growth Differ, 8, pp. 829-838, (1997)
[45]  
Symonds H., Krall L., Remington L., Saenz-Robles M., Lowe S., Jacks T., van Dyke T., p53-dependent apoptosis suppresses tumor growth and progression in vivo, Cell, 78, pp. 703-711, (1994)
[46]  
Howes K.A., Ransom N., Papermaster D.S., Lasudry J.G., Albert D.M., Windle J.J., Apoptosis or retinoblastoma: Alternative fates of photoreceptors expressing the HPV-16 E7 gene in the presence or absence of p53, Genes Dev, 8, pp. 1300-1310, (1994)
[47]  
Cui X.S., Donehower L.A., Differential gene expression in mouse mammary adenocarcinomas in the presence and absence of wild type p53, Oncogene, 19, pp. 5988-5996, (2000)
[48]  
Jones J.M., Cui X.S., Medina D., Donehower L.A., Heterozygosity of p21<sup>WAF1/CIP1</sup> enhances tumor cell proliferation and cyclin D1-associated kinase activity in a murine mammary cancer model, Cell Growth Differ, 10, pp. 213-222, (1999)
[49]  
Li B., Greenberg N., Stephens L.C., Meyn R., Medina D., Rosen J.M., Preferential overexpression of a 172Arg → Leu mutant p53 in the mammary gland of transgenic mice results in altered lobuloalveolar development, Cell Growth Differ, 5, pp. 711-721, (1994)
[50]  
Li B., Kittrell F.S., Medina D., Rosen J.M., Delay of dimethylbenz[a]anthracene-induced mammary tumorigenesis in transgenic mice by apoptosis induced by an unusual mutant p53 protein, Mol. Carcinog, 14, pp. 75-83, (1995)
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