Literature DB >> 18316601

A human breast cell model of preinvasive to invasive transition.

Aylin Rizki1, Valerie M Weaver, Sun-Young Lee, Gabriela I Rozenberg, Koei Chin, Connie A Myers, Jamie L Bascom, Joni D Mott, Jeremy R Semeiks, Leslie R Grate, I Saira Mian, Alexander D Borowsky, Roy A Jensen, Michael O Idowu, Fanqing Chen, David J Chen, Ole W Petersen, Joe W Gray, Mina J Bissell.   

Abstract

A crucial step in human breast cancer progression is the acquisition of invasiveness. There is a distinct lack of human cell culture models to study the transition from preinvasive to invasive phenotype as it may occur "spontaneously" in vivo. To delineate molecular alterations important for this transition, we isolated human breast epithelial cell lines that showed partial loss of tissue polarity in three-dimensional reconstituted basement membrane cultures. These cells remained noninvasive; however, unlike their nonmalignant counterparts, they exhibited a high propensity to acquire invasiveness through basement membrane in culture. The genomic aberrations and gene expression profiles of the cells in this model showed a high degree of similarity to primary breast tumor profiles. The xenograft tumors formed by the cell lines in three different microenvironments in nude mice displayed metaplastic phenotypes, including squamous and basal characteristics, with invasive cells exhibiting features of higher-grade tumors. To find functionally significant changes in transition from preinvasive to invasive phenotype, we performed attribute profile clustering analysis on the list of genes differentially expressed between preinvasive and invasive cells. We found integral membrane proteins, transcription factors, kinases, transport molecules, and chemokines to be highly represented. In addition, expression of matrix metalloproteinases MMP9, MMP13, MMP15, and MMP17 was up-regulated in the invasive cells. Using small interfering RNA-based approaches, we found these MMPs to be required for the invasive phenotype. This model provides a new tool for dissection of mechanisms by which preinvasive breast cells could acquire invasiveness in a metaplastic context.

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Year:  2008        PMID: 18316601      PMCID: PMC2662716          DOI: 10.1158/0008-5472.CAN-07-2225

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  54 in total

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2.  A role for dystroglycan in epithelial polarization: loss of function in breast tumor cells.

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3.  Why we're losing the war on cancer (and how to win it).

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Review 4.  Ductal carcinoma in situ of the breast.

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5.  beta4 integrin-dependent formation of polarized three-dimensional architecture confers resistance to apoptosis in normal and malignant mammary epithelium.

Authors:  Valerie M Weaver; Sophie Lelièvre; Johnathon N Lakins; Micah A Chrenek; Jonathan C R Jones; Filippo Giancotti; Zena Werb; Mina J Bissell
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6.  Tissue phenotype depends on reciprocal interactions between the extracellular matrix and the structural organization of the nucleus.

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Review 7.  Molecular alterations in ductal carcinoma in situ of the breast.

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Review 9.  Biological features of premalignant disease in the human breast.

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Authors:  Hong Liu; Derek C Radisky; Fei Wang; Mina J Bissell
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  78 in total

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2.  Laminin α5-derived peptides modulate the properties of metastatic breast tumour cells.

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Review 5.  Beyond 3D culture models of cancer.

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7.  Three-dimensional culture of human breast epithelial cells: the how and the why.

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9.  Regulation of membrane-type 4 matrix metalloproteinase by SLUG contributes to hypoxia-mediated metastasis.

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