The MUC1 Cytoplasmic Tail and Tandem Repeat Domains Contribute to Mammary Oncogenesis in FVB Mice

Christine L. Hattrup; Judy M. Bradley; Kari L. Kotlarczyk; Cathy S. Madsen; Cathy S. Madsen; Ronald J. Marler; Sandra J. Gendler

Breast Cancer: Basic and Clinical Research (Jan 2008)

The MUC1 Cytoplasmic Tail and Tandem Repeat Domains Contribute to Mammary Oncogenesis in FVB Mice

Christine L. Hattrup,
Judy M. Bradley,
Kari L. Kotlarczyk,
Cathy S. Madsen,
Cathy S. Madsen,
Ronald J. Marler,
Sandra J. Gendler

Affiliations

Christine L. Hattrup
Judy M. Bradley
Kari L. Kotlarczyk
Cathy S. Madsen
Cathy S. Madsen
Ronald J. Marler
Sandra J. Gendler

Journal volume & issue: Vol. 1
pp. 57 – 63

Abstract

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Background: Though the importance of the transmembrane mucin MUC1 in mammary oncogenesis has long been recognized, the relative contributions of the cytoplasmic tail and tandem repeat domains are poorly understood.Methods: To address this, mouse models of mammary carcinogenesis were created expressing full-length, cytoplasmic tail-deleted, or tandem repeat-deleted MUC1 constructs.Results: Overexpression of full-length MUC1 resulted in tumor formation in young mice (12 months); however, loss of either the cytoplasmic tail or the tandem repeat domain abrogated this oncogenic capacity. Aged mice in all strains developed late-onset mammary tumors similar to those previously described for the FVB background.Conclusions: This study is the fi rst spontaneous cancer model to address the relative importance of the cytoplasmic tail and tandem repeat domains to MUC1-driven mammary oncogenesis, and suggests that both of these domains are essential for tumor formation.

Published in Breast Cancer: Basic and Clinical Research

ISSN: 1178-2234 (Online)
Publisher: SAGE Publishing
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://journals.sagepub.com/home/bcb

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