4.8 Article

ErbB2, but not ErbB1, reinitiates proliferation and induces luminal repopulation in epithelial acini

Journal

NATURE CELL BIOLOGY
Volume 3, Issue 9, Pages 785-792

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/ncb0901-785

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Funding

  1. NCI NIH HHS [U54 CA143836, U01 CA143233-01, U01 CA143233, R01 CA057621-07, R01 CA064786, R01 CA057621, U54 CA126552-01, U54 CA112970, U54 CA143836-01, U54 CA126552, R01 CA064786-05, U54 CA112970-01] Funding Source: Medline

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Both ErbB1 and ErbB2 are overexpressed or amplified in breast tumours. To examine the effects of activating ErbB receptors in a context that mimics polarized epithelial cells in vivo, we activated ErbB1 and ErbB2 homodimers in preformed, growth-arrested mammary acini cultured in three-dimensional basement membrane gels. Activation of ErbB2, but not that of ErbB1, led to a reinitiation of cell proliferation and altered the properties of mammary acinar structures. These altered structures share several properties with early-stage tumours, including a loss of proliferative suppression, an absence of lumen, retention of the basement membrane and a lack of invasive properties. ErbB2 activation also disrupted tight junctions and the cell polarity of polarized epithelia, whereas ErbB1 activation did not have any effect. Our results indicate that ErbB receptors differ in their ability to induce early stages of mammary carcinogenesis in vitro and this three-dimensional model system can reveal biological activities of oncogenes that cannot be examined in vitro in standard transformation assays.

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