Characterization of Wnt-1 Transgenic Mice (with and without p53-deficiency) as Models of Spontaneous Mammary Tumorigenesis for Chemoprevention Studies.

Abstract

Wnt-1 transgenic(TG) mice develop mammary tumors at a high rate by 1 year of age due to mammary gland overexpression of the Wnt-1 oncogene. - We have shown that p53-deficiency accelerates mammary tumorigenesis in these mice, with 100% of p53-1- Wnt-1 TG mice and p53+/-Wnt-1 TG mice dead from mammary tumors by 5 months and 9 months of age, respectively. To test their response to cancer preventive regimens, we randomized 104 female p53+/- Wnt-1 TG mice (5 weeks of age, 20 mice/treatment) to receive: 1) control diet (AIN-76A diet); 2) fenretinide (AIN 76A diet with 0.04% w/w fenretinide); 3) fluasterone (AIN- 76A diet with 0.2% fluasterone); 4) soy (AIN-76A diet with 0.45% phytochemical-enriched soy extract); or 5) a calorie restriction regimen (40% reduction in carbohydrate calorie intake relative to the control group). All mice were euthanized once a tumor reached 1.5 cm in diameter. We found that, relative to the control group (MTD=15.7 weeks), the fenretinide (MTD=23.1 weeks, p=O.Ol) and fluasterone (MTD=23.l weeks, p=O.006) and soy (MTD =21 weeks, p=O.04) groups displayed moderate but significant delays in tumor development and death, while the calorie restricted group (MTD > 40 weeks; p<O.OOl) experienced highly significant delays in spontaneous mammary tumor development. Similar trends were observed with these agents in male and female pS3-/- Wnt-l TG mice and female p53+/+ Wnt-l TG mice; however, the forrner genotype appears to develop mammary tumors too rapidly to be an effective model while the latter genotype is too slow and variable relative to the p53+/- Wnt-1 TG mice. We conclude that pS3+/- Wnt-1 TG mice provide a rapid and sensitive model of spontaneous mammary tumorigenesis for characterizing breast cancer prevention strategies.

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Document Details

Document Type
Technical Report
Publication Date
Sep 01, 1998
Accession Number
ADA366651

Entities

People

  • Stephen D. Hursting

Organizations

  • Joint Publications Research Service

Tags

DTIC Thesaurus Topics

  • Abstracts
  • Biomedical Research
  • Body Weight
  • Breast Cancer
  • Cancer
  • Carbohydrates
  • Cell Physiological Processes
  • Cells
  • Deficiencies
  • Drug Therapy
  • Genes
  • Genetics
  • Lymphocytes
  • Mammary Glands
  • Medical Personnel
  • Neoplasms
  • Oncology

Fields of Study

  • Biology

Readers

  • Molecular Biology and Genetics
  • Toxicology/Environmental Toxicology
  • Women's Health and Cancer Risk Research: African American Women and Pregnancy Outcomes.

Technology Areas

  • Biotechnology