Development of a Transgenic Mouse Model for Breast Cancer that is Optimized for the Study of T Cell-Based Therapeutic Strategies

Abstract

We sought to develop a transgenic mouse model for breast cancer that would allow the in viva activities of tumor-specific T cell clones to be tracked through all stages of tumorigenesis and after various - immunotherapies. We "tagged" the neu oncogene with two defined T cell epitopes which conferred recognition by OT-l and OT-II T cell receptor (TOR) transgenic T cells. When expressed as a transgenic in mammary epithelium, epitope-tagged neu (designated neu(subOTl/OT2) was expected to induce mammary adenocarcinomas that express the epitope tags and hence are recognizable by OT-l and OT-II T cells. We generated three neu(subOTl/OT2) transgene-positive founder lines, and expression of neu(subOTl/OT2) in mammary epithelium was confirmed by Northern blot, western blot, and by immunological responses to the epitope tags. On its own, neu(subOTl/OT2) induced tumors in a minority of mice and with a long latency (12-16 months). Fortunately, when neu(subOTl/OT2) mice were crossed to mice expressing a mutant p53 transgene, tumors developed in the majority (718) of mice with a reasonable latency (7-9.5 months). We are currently using this model to analyze the T cell response to spontaneous mammary tumors and to develop novel immunotherapies for breast cancer. Thus, we fully accomplished the goals of this project.

Document Details

Document Type

Technical Report

Publication Date

Jun 01, 2004

Accession Number

ADA425600

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