Your search keyword '"Murphy, Kristen L."' showing total 4 results

1. Mutant p53 and genomic instability in a transgenic mouse model of breast cancer

Author

Murphy, Kristen L and Rosen, Jeffrey M

Published

2000

2. Bcl-2 expression delays mammary tumor development in dimethylbenz(a)anthracene-treated transgenic mice

Author

Murphy, Kristen L, Kittrell, Frances S, Gay, Jason P, Jäger, Richard, Medina, Daniel, and Rosen, Jeffrey M

Published

1999

3. Cooperative interaction between mutant p53 and des(1-3)IGF-I accelerates mammary tumorigenesis.

Author

Hadsell, Darryl L, Murphy, Kristen L, Bonnette, Sharon G, Reece, Naomi, Laucirica, Rodolfo, and Rosen, Jeffrey M

Subjects

*TRANSGENIC mice, *APOPTOSIS, *CARCINOGENESIS

Abstract

Mammary tumorigenesis was analysed in transgenic mice which overexpress des(1-3)hIGF-I (WAP-DES) and/or a mutant form of p53 (p53172R-H). Nonlactating, multiparous WAP-DES mice exhibited hyperplastic lesions termed mammary interepithelial neoplasia (MIN) which constitutively expressed WAP-DES. By 23 months of age, 53% of the WAP-DES mice developed mammary adenocarcinomas. A 75% reduction in both apoptosis and proliferation was observed in the normal mammary glands of WAP-DES mice. Mammary tumor incidence in WAP-DES/p53 bitransgenic mice was similar to that of WAP-DES and 2–3-fold greater than that of nontransgenic and p53172R-H females. Tumor latency, however, was reduced by 8 months in bitransgenic mice as compared to mice of the other three genotypes. Aneuploidy was frequently observed in tumors from bitransgenic and p53172R-H mice, but not from mice expressing only the WAP-DES transgene. Expression of IGFBP3 was elevated in tumors from WAP-DES, but not bitransgenic mice, indicating an alteration in the p53/IGF-I axis. These studies indicate that overexpression of des(1-3)hIGF-I increases the frequency of MIN and stochastic mammary tumors and that the appearance of tumors displaying genomic instability is accelerated by mutant p53172R-H. Oncogene (2000) 19, 889–898. [ABSTRACT FROM AUTHOR]

Published

2000

4. A transgenic mouse model for mammary carcinogenesis.

Author

Li, Baolin, Murphy, Kristen L, Laucirica, Rodolfo, Kittrell, Frances, Medina, Daniel, and Rosen, Jeffrey M

Subjects

*BREAST cancer, *TRANSGENIC mice, *TUMOR suppressor genes

Abstract

Missense mutations in the p53 tumor suppressor occur frequently in human breast cancer and influence both the prognosis and response to chemotherapy. Amino acid 175 (equivalent to murine 172) is the second most common site of missense mutations in p53 in human breast cancer. Over 95% of these mutations are arginine-to-histidine (R-H) substitutions resulting in a gain-of-function, and not merely a dominant-negative phenotype. Transgenic mice expressing a p53 172R–H construct targeted to the mammary gland by means of a whey acidic protein (WAP) promoter were characterized as a model system in order to determine the specific effects of this mutation on mammary tumorigenesis. Although transgene expression alone had no apparent effect on normal mammary development, transgenic mice treated with the chemical carcinogen dimethylbenz(a)anthracene developed tumors with much shorter latency than did control littermates and had a greater tumor burden. Tumors arising in transgenic mice did not exhibit either decreased apoptosis or increased cell proliferation relative to tumors arising in nontransgenic littermates, but did display increased genomic instability. Large pleiomorphic nuclei were visible in many tumors from transgenic mice, and DNA flow analysis confirmed the presence of significant aneuploid cell populations. Since these transgenic mice develop very few spontaneous tumors, while accelerating carcinogen-and oncogene-mediated tumorigenesis, this mouse model will, therefore, be useful in the investigation of early events in mammary tumorigenesis. It may also be used as a preclinical model to test newly developed chemotherapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

1998