Correlation between MMPs and their inhibitors in breast cancer tumor tissue specimens and in cell lines with different metastatic potential

Figueira, R.C.S.; Gomes, Luciana Rodrigues; Neto, João Siufi; Silva, Fabricio C; Silva, Ismael D.C.G.; Sogayar, Mari Cleide

doi:10.1186/1471-2407-9-20

Cited by 116 publications

(112 citation statements)

References 35 publications

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“…56,57 The expression and activity of MMPs has been linked to advanced stages of breast cancer, greater tumor invasion and the construction of metastatic formations. 58,59,60 Some studies have highlighted the importance of matrix MMP expression by stromal cells as a prognostic factor in the TNBC subtype. 61 These molecules are thus attractive targets for drug development.…”

Section: Discussionmentioning

confidence: 99%

Biological network-driven gene selection identifies a stromal immune module as a key determinant of triple-negative breast carcinoma prognosis

et al. 2015

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Triple-negative breast cancer (TNBC) is a heterogeneous group of aggressive breast cancers for which no targeted treatment is available. Robust tools for TNBC classification are required, to improve the prediction of prognosis and to develop novel therapeutic interventions. We analyzed 3,247 primary human breast cancer samples from 21 publicly available datasets, using a five-step method: (1) selection of TNBC samples by bimodal filtering on ER-HER2 and PR, (2) normalization of the selected TNBC samples, (3) selection of the most variant genes, (4) identification of gene clusters and biological gene selection within gene clusters on the basis of String© database connections and gene-expression correlations, (5) summarization of each gene cluster in a metagene. We then assessed the ability of these metagenes to predict prognosis, on an external public dataset (METABRIC). Our analysis of gene expression (GE) in 557 TNBCs from 21 public datasets identified a six-metagene signature (167 genes) in which the metagenes were enriched in different gene ontologies. The gene clusters were named as follows: Immunity1, Immunity2, Proliferation/DNA damage, AR-like, Matrix/Invasion1 and Matrix2 clusters respectively. This signature was particularly robust for the identification of TNBC subtypes across many datasets (n D 1,125 samples), despite technology differences (Affymetrix© A, Plus2 and Illumina©). Weak Immunity two metagene expression was associated with a poor prognosis (disease-specific survival; HR D 2.68 [1.59-4.52], p D 0.0002). The six-metagene signature (167 genes) was validated over 1,125 TNBC samples. The Immunity two metagene had strong prognostic value. These findings open up interesting possibilities for the development of new therapeutic interventions.

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Section: Discussionmentioning

confidence: 99%

Biological network-driven gene selection identifies a stromal immune module as a key determinant of triple-negative breast carcinoma prognosis

et al. 2015

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“…In addition to its catalytic domain, MMP-14 contains a short cytoplasmic sequence that is involved in the regulation of the enzyme activity and in the activation of signal transduction processes (Gingras and Be´liveau, 2010). MMP-14 is overexpressed in many types of tumors, including breast carcinomas (Okada et al, 1995;Figueira et al, 2009), where it constitutes an independent predictor of adverse outcome (McGowan and Duffy, 2008).…”

Section: Introductionmentioning

confidence: 99%

MT1-MMP protects breast carcinoma cells against type I collagen-induced apoptosis

et al. 2011

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As invading breast carcinoma cells breach their underlying basement membrane, they become confronted with a dense three-dimensional reactive stroma dominated by type I collagen. To develop metastatic capabilities, invading tumor cells must acquire the capacity to negotiate this novel microenvironment. Collagen influences the fate of epithelial cells by inducing apoptosis. However, the mechanisms used by invading tumor cells to evade collagen-induced apoptosis remain to be defined. We demonstrate that membrane type-1 matrix metalloproteinase (MT1-MMP/MMP-14) confers breast cancer cells with the ability to escape apoptosis when embedded in a collagen gel and after orthotopic implantation in vivo. In the absence of MMP-14-dependent proteolysis, type I collagen triggers apoptosis by inducing the expression of the pro-apoptotic Bcl-2-interacting killer in luminallike breast cancer cells. These findings reveal a new mechanism whereby MMP-14 activity promotes tumor progression by circumventing apoptosis.

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“…Increased MT1-MMP expression is more frequently associated with poor outcome in patients who are lymph node and metastases positive for disease (Figueira et al, 2009;Jiang et al, 2006;Kim et al, 2006;Ueno et al, 1997), and increased VEGF-A is also associated with poor prognosis and correlates with MT1-MMP expression (Linderholm et al, 2003;Munaut et al, 2003), suggesting the MT1-MMP-VEGF-A axis might be a key element in tumour progression. An improvement in our understanding of how the VEGF-A-VEGFR-2 axis functions in pathology is of particular importance as inhibitors of the VEGF axis have recently been shown to increase tumorigenicity at metastatic sites in murine models of cancer, which parallels observations emerging from clinical data (Ebos et al, 2009;Paez-Ribes et al, 2009).…”

Section: The Mt1-mmp Extracellular Domains Are Important For Expressimentioning

confidence: 99%

MT1-MMP regulates VEGF-A expression through a complex with VEGFR-2 and Src

Eisenach

Roghi

Fogarasi

et al. 2010

Journal of Cell Science

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SummaryMembrane-type-1 matrix metalloproteinase (MT1-MMP) is a zinc-dependent type-I transmembrane metalloproteinase involved in pericellular proteolysis, migration and invasion, with elevated levels correlating with a poor prognosis in cancer. MT1-MMP-mediated transcriptional regulation of genes in cancer cells can contribute to tumour growth, although this is poorly understood at a mechanistic level. In this study, we investigated the mechanism by which MT1-MMP regulates the expression of VEGF-A in breast cancer cells. We discovered that MT1-MMP regulates VEGFR-2 cell surface localisation and forms a complex with VEGFR-2 and Src that is dependent on the MT1-MMP hemopexin domain and independent of its catalytic activity. Although the localisation of VEGFR-2 was independent of the catalytic and intracellular domain of MT1-MMP, intracellular signalling dependent on VEGFR-2 activity leading to VEGF-A transcription still required the MT1-MMP catalytic and intracellular domain, including residues Y573, C574 and DKV582. However, there was redundancy in the function of the catalytic activity of MT1-MMP, as this could be substituted with MMP-2 or MMP-7 in cells expressing inactive MT1-MMP. The signalling cascade dependent on the MT1-MMP-VEGFR-2-Src complex activated Akt and mTOR, ultimately leading to increased VEGF-A transcription.

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Correlation between MMPs and their inhibitors in breast cancer tumor tissue specimens and in cell lines with different metastatic potential

Cited by 116 publications

References 35 publications

Biological network-driven gene selection identifies a stromal immune module as a key determinant of triple-negative breast carcinoma prognosis

Biological network-driven gene selection identifies a stromal immune module as a key determinant of triple-negative breast carcinoma prognosis

MT1-MMP protects breast carcinoma cells against type I collagen-induced apoptosis

MT1-MMP regulates VEGF-A expression through a complex with VEGFR-2 and Src

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