Matrix Metalloproteinase-Induced Epithelial-Mesenchymal Transition in Breast Cancer

Radisky, Evette S.; Radisky, Derek C.

doi:10.1007/s10911-010-9177-x

Cited by 418 publications

(363 citation statements)

References 144 publications

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“…Consistent with this idea, gain in hSETD1A gene copy number is detected in approximately 45% of breast tumors (39). Finally, increased MMP activity is commonly observed in breast cancer cells and promotes a variety of cellular activities including proliferation, migration, and invasion (33,(40)(41)(42)(43). Taken together, these facts prompted us to investigate a possible link between hSETD1A, H3K4me3, MMP expression, and metastatic breast cancer phenotype.…”

Section: Introductionmentioning

confidence: 69%

“…MMPs are widely known as critically important in promoting cancer cell migration and invasion by degrading extracellular matrix proteins (33,(40)(41)(42)(43). As previous work from our group indicated that hSETD1A was required for MMP7 expression in colorectal tumor lines (26), we examined a number of MMP genes that could be potentially affected by hSETD1A knockdown in breast cancer cells.…”

Section: Discussionmentioning

confidence: 99%

“…MMPs are enzymes which catalyze degradation of extracellular matrix components and are secreted by cells within the tumor microenvironment and/or by the tumor cells themselves. This activity promotes cancer cell invasion, migration, and proliferation, and associates with poorer survival in breast cancer (33,(40)(41)(42)(43).…”

Section: Hsetd1a Knockdown Reduces Metastasis In Nude Micementioning

confidence: 99%

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Histone Methyltransferase hSETD1A Is a Novel Regulator of Metastasis in Breast Cancer

Salz

Deng

Pampo

et al. 2015

Molecular Cancer Research

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Epigenetic alteration is a hallmark of all cancers. Such alterations lead to modulation of fundamental cancer-related functions, such as proliferation, migration, and invasion. In particular, methylation of Histone H3 Lysine 4 (H3K4), a histone mark generally associated with transcriptional activation, is altered during progression of several human cancers. While the depletion of H3K4 demethylases promotes breast cancer metastasis, the effect of H3K4 methyltransferases on metastasis is not clear. Nevertheless, gene duplications in the human SETD1A (hSETD1A) H3K4 methyltransferase are present in almost half of breast cancers. Herein, expression analysis determined that hSETD1A is upregulated in multiple metastatic human breast cancer cell lines and clinical tumor specimens. Ablation of hSETD1A in breast cancer cells led to a decrease in migration and invasion in vitro and to a decrease in metastasis in nude mice. Furthermore, a group of matrix metalloproteinases (including MMP2, MMP9, MMP12, MMP13, and MMP17) were identified which were downregulated upon depletion of hSETD1A and demonstrated a decrease in H3K4me3 at their proximal promoters based on chromatin immunoprecipitation analysis. These results provide evidence for a functional and mechanistic link among hSETD1A, MMPs, and metastasis in breast cancer, thereby supporting an oncogenic role for hSETD1A in cancer.Implications: This study reveals that hSETD1A controls tumor metastasis by activating MMP expression and provides an epigenetic link among hSETD1A, MMPs, and metastasis of breast cancer.

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Section: Introductionmentioning

confidence: 69%

Section: Discussionmentioning

confidence: 99%

Section: Hsetd1a Knockdown Reduces Metastasis In Nude Micementioning

confidence: 99%

See 1 more Smart Citation

Histone Methyltransferase hSETD1A Is a Novel Regulator of Metastasis in Breast Cancer

Salz

Deng

Pampo

et al. 2015

Molecular Cancer Research

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“…Another group of molecules with the ability to induce EMT in physiological and pathological conditions are the metalloproteinases (MMP) (reviewed in [51]). The role of MMPs as EMT inducers has been described in kidney, lung, ovary, oral, and mammary epithelium [52][53][54][55][56][57].…”

Section: The Epithelium To Mesenchymal Transitionmentioning

confidence: 99%

Nucleotides and nucleoside signaling in the regulation of the epithelium to mesenchymal transition (EMT)

Martinez-Ramirez

Dı́az-Muñoz

Butanda-Ochoa

et al. 2016

Purinergic Signalling

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The epithelium-mesenchymal transition (EMT) is an important process of cell plasticity, consisting in the loss of epithelial identity and the gain of mesenchymal characteristics through the coordinated activity of a highly regulated informational program. Although it was originally described in the embryonic development, an important body of information supports its role in pathology, mainly in cancerous and fibrotic processes. The purinergic system of inter-cellular communication, mainly based in ATP and adenosine acting throughout their specific receptors, has emerged as a potent regulator of the EMT in several pathological entities. In this context, cellular signaling associated to purines is opening the understanding of a new element in the complex regulatory network of this phenotypical differentiation process. In this review, we have summarized recent information about the role of ATP and adenosine in EMT, as a growing field with high therapeutic potential.Keywords P2 receptors . P1 receptors . Purinergic signaling . Cell migration . EMTThe purinergic system of intercellular communication General aspects The term purine (from: pure urine) was created more than 130 years ago by Emil Fischer after detailed analytical characterization of the uric acid molecule [1]. Purine molecular structure is the result of fusing pyrimidine and imidazole rings, and it exists as four N-H tautomeric forms [2]. Tautomerism of purine bases in DNA is one of the earliest reasons for mutations [3][4][5]. The interconversion of the different adenine or guanine tautomers produced mispairing with pyrimidines (which also show tautomeric forms) that may lead to changes in DNA sequence [6].Purine molecules appeared very early in the history of our planet, in the period known as Borganic evolution^, before the establishment of living systems. It has been postulated that purines could be formed by a eutectic (denoting a mixture of substances in fixed proportions that melts and freezes at a single temperature that is lower than the melting points of any of the separate constituents) concentration of HCN at extremely low temperature over a period of dozens of years [7]. Purine molecules, such as adenine and guanine, are components of the genetic material (DNA and RNA) of all living beings. Purine and pyrimidine tautomeric equilibria in nucleic acids was postulated to be significant in events such as DNA replication and repair as well as in the occurrence of point mutations [8].As nucleosides and nucleotides, purines play other highly strategic roles, acting as energy intermediates, allosteric regulators of key metabolic activities, redox molecules, and chemical messengers for signal transduction events. The two most important purines serving as extracellular ligands for paracrine and autocrine signaling are ATP and its dephosphorylated form, adenosine (ADO). ATP and ADO act as intracellular intermediate metabolites, and their presence in the

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“…8,9 Identifying proteases that drive tumor progression and metastasis, and defining their specific mechanisms of action, can potentially reveal novel druggable targets and underexplored avenues for slowing or halting the spread of metastatic disease. 10 Moreover, as extracellular molecules with binding sites for highly specific substrate ligands, secreted proteases are more amenable to pharmacological inhibition that are many oncogenic signaling pathways within the cell.…”

mentioning

confidence: 99%

PRSS3/mesotrypsin in prostate cancer progression: implications for translational medicine

Radisky¹

2013

Asian J Androl

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Matrix Metalloproteinase-Induced Epithelial-Mesenchymal Transition in Breast Cancer

Cited by 418 publications

References 144 publications

Histone Methyltransferase hSETD1A Is a Novel Regulator of Metastasis in Breast Cancer

Histone Methyltransferase hSETD1A Is a Novel Regulator of Metastasis in Breast Cancer

Nucleotides and nucleoside signaling in the regulation of the epithelium to mesenchymal transition (EMT)

PRSS3/mesotrypsin in prostate cancer progression: implications for translational medicine

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