Exogenous expression of N-cadherin in breast cancer cells induces cell migration, invasion, and metastasis Journal Article

   


Authors: Hazan, R. B.; Phillips, G. R.; Qiao, R. F.; Norton, L.; Aaronson, S. A.
Article Title: Exogenous expression of N-cadherin in breast cancer cells induces cell migration, invasion, and metastasis
Abstract: E- and N-cadherin are calcium-dependent cell adhesion molecules that mediate cell-cell adhesion and also modulate cell migration and tumor invasiveness. The loss of E-cadherin-mediated adhesion has been shown to play an important role in the transition of epithelial tumors from a benign to an invasive state. However, recent evidence indicates that another member of the cadherin family, N-cadherin, is expressed in highly invasive tumor cell lines that lacked E-cadherin expression. These findings have raised the possibility that N-cadherin contributes to the invasive phenotype. To determine whether N-cadherin promotes invasion and metastasis, we transfected a weakly metastatic and E-cadherin-expressing breast cancer cell line, MCF-7, with N-cadherin and analyzed the effects on cell migration, invasion, and metastasis. Transfected cells expressed both E- and N-cadherin and exhibited homotypic cell adhesion from both molecules. In vitro, N-cadherin-expressing cells migrated more efficiently, showed an increased invasion of Matrigel, and adhered more efficiently to monolayers of endothelial cells. All cells produced low levels of the matrix metalloproteinase MMP-9, which was dramatically upregulated by treatment with FGF-2 only in N-cadherin-expressing cells. Migration and invasion of Matrigel were also greatly enhanced by this treatment. When injected into the mammary fat pad of nude mice, N-cadherin-expressing cells, but not control MCF-7 cells, metastasized widely to the liver, pancreas, salivary gland, omentum, lung, lymph nodes, and lumbar spinal muscle. The expression of both E- and N-cadherin was maintained both in the primary tumors and metastatic lesions. These results demonstrate that N-cadherin promotes motility, invasion, and metastasis even in the presence of the normally suppressive E-cadherin. The increase in MMP-9 production by N-cadherin-expressing cells in response to a growth factor may endow them with a greater ability to penetrate matrix protein barriers, while the increase in their adherence to endothelium may improve their ability to enter and exit the vasculature, two properties that may be responsible for metastasis of N-cadherin-expressing cells.
Keywords: controlled study; protein expression; human cell; nonhuman; animal cell; mouse; animals; mice; metastasis; breast cancer; gene expression; gelatinase b; animal experiment; cancer cell culture; tumor cells, cultured; transfection; breast neoplasms; uvomorulin; cancer invasion; fibroblast growth factor 2; genetic transfection; endothelium, vascular; mice, nude; nerve cell adhesion molecule; neoplasm metastasis; collagen; cell migration; cell movement; epithelial cells; neoplasm invasiveness; neoplasm transplantation; drug combinations; cell adhesion; cadherins; motility; laminin; e-cadherin; enzyme induction; matrix metalloproteinase 9; mmp-9; proteoglycans; humans; human; female; priority journal; article; fgf-2
Journal Title: Journal of Cell Biology
Volume: 148
Issue: 4
ISSN: 0021-9525
Publisher: Rockefeller University Press  
Date Published: 2000-02-21
Start Page: 779
End Page: 790
Language: English
DOI: 10.1083/jcb.148.4.779
PUBMED: 10684258
PROVIDER: scopus
PMCID: PMC2169367
DOI/URL:

http://www.scopus.com/inward/record.url?eid=2-s2.0-0034695913&partnerID=40&md5=6e60240813b0a531a52b633d9a732e85
Notes: Export Date: 18 November 2015 -- Source: Scopus
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MSK Authors
  1. Larry Norton
    736 Norton
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