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This article is part of the supplement: Breast cancer research: the past and the future

Poster Presentation

Functional analysis of normal and DCIS modified breast myoepithelial cells

M Allen, K Mulligan, S Clark, I Hart, JF Marshall and JL Jones

Institute of Cancer, Centre for Tumour Biology, Barts and London, Queen Mary, University of London, UK

from Breast cancer research: the past and the future
London, UK. 1 November 2006

Breast Cancer Research 2006, 8(Suppl 2):P14doi:10.1186/bcr1569

Published: 1 November 2006

© 2006 BioMed Central Ltd

Background

Normal breast myoepithelial cells have been shown to exhibit tumour-suppressor activity mediated, in part, by downregulation of MMP expression [1]. DCIS myoepithelial cells have an altered phenotype as demonstrated by a different gene expression profile [2]. We have identified upregulation of α(v)β6 integrin on myoepithelial cells in a subset of DCIS; however, the role of α(v)β6 in this context is not clear. α(v)β6 is not expressed by normal epithelial cells, but is expressed in some cancers where it promotes tumour cell invasion and enhances MMP expression.

Methods

The purpose of this project is to investigate the hypothesis that DCIS-associated myoepithelial cells lose their tumour suppressor effect and acquire a tumour promoting activity. There are three general aims: (1) to generate a series of myoepithelial cell models to mimic DCIS-associated myoepithelial cells and overexpress α(v)β6 to assess the contribution of this integrin; (2) to compare tumour suppressor/promoter properties of normal, α(v)β6 overexpressing and DCIS-associated myoepithelial cells; and (3) to examine the effect of de novo α(v)β6 expression on the biological activity of myoepithelial cells.

Results

We have fully characterised an immortalised myoepithelial cell line, engineered it to overexpress α(v)β6 and determined that it is functional. We are starting to examine the morphology and phenotype of these cells to determine any differences, and we have been able to show the parental cell line is able to recapitulate the tumour suppressor effect in in vitro systems. We are now looking into what effect the expression of α(v)β6 has in these systems. We are also in the process of trying to create further myoepithelial cell lines from primary cells isolated from patient tissue.

Conclusion

Through this work we hope to identify the role α(v)β6 expression has in DCIS myoepithelial cells with the goal of making this integrin a viable therapeutic target in the future.

Acknowledgements

This work was funded by Breast Cancer Campaign.

References

  1. Jones J, Shaw J, Pringle J, Wlaker R: Primary breast myoepithelial cells exert an invasion-suppressor effect on breast cancer cells via paracrine down-regulation of MMP expression in fibroblasts and tumour cells.

    J Pathol 2003, 201:562-572. PubMed Abstract | Publisher Full Text OpenURL

  2. Allinen M, Beroukhim R, Cai L, et al.: Molecular characterization of the tumor microenvironment in breast cancer.

    Cancer Cell 2004, 6:17-32. PubMed Abstract | Publisher Full Text OpenURL

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