Suppression of Integrin α3β1 in Breast Cancer Cells Reduces <i>Cyclooxygenase-2</i> Gene Expression and Inhibits Tumorigenesis, Invasion, and Cross-Talk to Endothelial Cells

Mitchell, Kara; Svenson, Kimberly B.; Longmate, Whitney; Gkirtzimanaki, Katerina; Sądej, Rafał; Wang, Xianhui; Zhao, Jihe; Eliopoulos, Aristides G.; Berditchevski, Fedor; DiPersio, C. Michael

doi:10.1158/0008-5472.can-09-4283

Cited by 80 publications

(126 citation statements)

References 48 publications

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“…5B and 5C). It has been reported that integrin ␣3␤1 promotes radiation-induced migration of meningioma cells and that suppression of integrin ␣3␤1 inhibits tumorigenesis and invasion in breast cancer cells (66). Our transwell assay on the ITGA3 knockdown cells also supported the same conclusion.…”

Section: Analysis Of Identified Glycoproteins Enriched Via Erlic-supporting

confidence: 87%

Hypoxia-induced Changes to Integrin α 3 Glycosylation Facilitate Invasion in Epidermoid Carcinoma Cell Line A431

Ren

Hao

Law

et al. 2014

Molecular & Cellular Proteomics

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Hypoxia is a critical microenvironmental factor that drives cancer progression through angiogenesis and metastasis. Glycoproteins, especially those on the plasma membrane, orchestrate this process; however, questions remain regarding hypoxia-perturbed protein glycosylation in cancer cells. We focused on the effects of hypoxia on the integrin family of glycoproteins, which are central to the cellular processes of attachment and migration and have been linked with cancer in humans. We employed electrostatic repulsion hydrophilic interaction chromatography coupled with iTRAQ labeling and LC-MS/MS to identify and quantify glycoproteins expressed in A431. The results revealed that independent of the protein-level change, N-glycosylation modifications of integrin ␣ 3 (ITGA3) were inhibited by hypoxia, unlike in other integrin subunits. A combination of Western blot, flow cytometry, and cell staining assays showed that hypoxia-induced alterations to the glycosylation of ITGA3 prevented its efficient translocation to the plasma membrane. Mutagenesis studies demonstrated that simultaneous mutation of glycosites 6 and 7 of ITGA3 prevented its accumulation at the K562 cell surface, which blocked integrin ␣ 3 and ␤ 1 heterodimer formation and thus abolished ITGA3's interaction with extracellular ligands. By generating A431 cells stably expressing ITGA3 mutated at glycosites 6 and 7, we showed that lower levels of ITGA3 on the cell surface, as induced by hypoxia, conferred an increased invasive ability to cancer cells in vitro under hypoxic conditions. Taken together, these results revealed that ITGA3 translocation to the plasma membrane suppressed by hypoxia through inhibition of glycosylation facilitated cell invasion in A431. Molecular & Cellular Proteomics 13: 10.1074/mcp.M114.038505, 3126-3137, 2014.As solid tumors grow, those areas distant from the existing blood vessels can become chronically or intermittently deprived of sufficient oxygen. These hypoxic conditions place tremendous pressure on tumor cells and drive the development of increasingly malignant and metastatic phenotypes (1, 2). As metastases are responsible for more than 90% of human cancer-related deaths, much research has aimed to define the underlying molecular mechanisms of the tumor cell response to a hypoxic microenvironment (3-5). However, despite the evident clinical relevance of metastasis, the full complexity of the process remains incompletely understood. An emerging area of interest is the importance of the carbohydrate structures in tumor cells, which have been linked to control of protein folding and stability, cell-cell recognition, adhesion, invasion, and metastatic potentials (6 -11). The post-translational enzymatic addition of glycans (glycosylation) to proteins is a potent modulator of the functions of many receptors involved in cell growth, adhesion, and signal transduction (11)(12)(13)(14) and is commonly seen in both in vitro and in vivo cancer models (15, 16). Furthermore, a growing body of studies has shown a clear correlation betw...

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Section: Analysis Of Identified Glycoproteins Enriched Via Erlic-supporting

confidence: 87%

Hypoxia-induced Changes to Integrin α 3 Glycosylation Facilitate Invasion in Epidermoid Carcinoma Cell Line A431

Ren

Hao

Law

et al. 2014

Molecular & Cellular Proteomics

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“…Preclinical studies have shown that a3b1 promotes malignant behavior of breast cancer cells in vivo and in vitro (Cagnet et al, 2013;Mitchell et al, 2010;Morini et al, 2000;Scales et al, 2013;Sugiura and Berditchevski, 1999;Wang et al, 2004), as well as skin tumorigenesis in vivo (Sachs et al, 2012), implicating this integrin as a potential therapeutic target to inhibit cancer progression and metastasis (Subbaram and DiPersio, 2011). Laminin-332, a major ECM ligand for a3b1, is often expressed highly in breast cancer cells, where it enhances motility (Carpenter et al, 2009;Carpenter et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

“…Laminin-332, a major ECM ligand for a3b1, is often expressed highly in breast cancer cells, where it enhances motility (Carpenter et al, 2009;Carpenter et al, 2008). At least some functions of a3b1 in transformed or immortalized cells are attributable to the ability of a3b1 to regulate genes that stimulate invasive growth and/or angiogenesis, including matrix metalloproteinase-9 (MMP-9) (Iyer et al, 2005;Morini et al, 2000) and cyclooxygenase (Cox-2, also known as prostaglandin G/H synthase 2 in human) (Mitchell et al, 2010). In immortalized keratinocytes, a3b1-dependent-induction of MMP-9 occurs through a post-transcriptional mechanism of enhanced mRNA stability (Iyer et al, 2005).…”

Section: Introductionmentioning

confidence: 99%

“…We previously showed that stable, shRNA-mediated suppression of a3b1 in MDA-MB-231 breast cancer cells reduced expression of the Cox-2 gene and abrogated tumor growth in an orthotopic model (Mitchell et al, 2010). To determine whether acute suppression of a3b1 similarly reduces Cox-2 expression, and whether this regulation extends to other breast cancer lines, we transfected MDA-MB-231 cells or MCF7 cells each with two different siRNAs that target the a3 integrin subunit (hereafter referred to as a3).…”

Section: Introductionmentioning

confidence: 99%

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Integrin α3β1 controls mRNA splicing that determines cyclooxygenase-2 (Cox-2) mRNA stability in breast cancer cells

Subbaram

Lyons

Svenson

et al. 2014

Journal of Cell Science

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It is unknown how cues from the tumor microenvironment can regulate post-transcriptional mechanisms, such as alternative splicing, that control genes that drive malignant growth. The induction of cyclooxygenase 2 (Cox-2) by integrin a3b1 in breast cancer cells can promote tumor progression. We have used RNAi to suppress a3b1 in human MDA-MB-231 breast cancer cells and then investigated changes in global gene expression. Numerous mRNAs, including Cox-2, show altered expression and/or alternative exon usage (AEU) in a3b1-deficient cells. AEU included patterns predicted to render an mRNA susceptible to degradation, such as 39-UTR variations or retention of elements that target an mRNA for nonsense-mediated decay (NMD). PCR-based analysis of a3b1-deficient cells confirmed changes in Cox-2 mRNA that might target it for NMD, including retention of an intron that harbors premature termination codons and changes within the 39-UTR. Moreover, Cox-2 mRNA has reduced stability in a3b1-deficient cells, which is partially reversed by knockdown of the essential NMD factor UPF1. Our study identifies a3b1-mediated AEU as a novel paradigm of integrin-dependent gene regulation that has potential for exploitation as a therapeutic target.

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“…COX-2 is an inducible enzyme that interferes with tumor development and angiogenesis, related to the inhibition of apoptosis through inhibition of the proapoptotic Bax protein and overexpression of the antiapoptotic bcl-2 protein. COX-2 catalyzes the conversion of arachidonic acid to PGE2 and enhances the metastatic phenotype of both breast cancer cells in vitro and breast tumors (Mitchell et al, 2010;Miglietta et al, 2010). PGE2, the catalytic product of COX-2, may promote tumor development and angiogenesis (Boland et al, 2004;Miglietta et al, 2010;Yu et al, 2014).…”

Section: Discussionmentioning

confidence: 99%

COX-2 expression correlation with invasion in human breast carcinomas and in cell line MDA-MB-231 in vitro

Wang

Chen

et al. 2016

Bangladesh J Pharmacol

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COX-2 expression by means of immunohistochemistry in 120 cases breast invasive ductal carcinomas and 60 cases benign lesions were compared with clinicopathological features and prognostic molecular markers. COX-2 role of invasiveness and chemotaxis in breast cancer cell line MDA-MB-231 by using small RNA interference (siRNA) plasmids to disrupt COX-2 expression in vitro were investigated. The results show that COX-2 immune positivity and percentage of positive cells in breast carcinomas were higher than those in benign lesions and positivity correlated significantly with HIF-1?, VEGF, the grading, metastasis and vascular invasion of carcinoma (p<0.05). This study suggests that COX-2 overexpression correlates with poor clinicopathological parameters in breast cancers, and the reduction of COX-2 expression can obviously inhibit the invasion and chemotaxis of cancer cell line MDA-MB-231 using RNA interference. The findings of the present study suggest that COX-2 overexpression in breast cancer may be considered as a negative prognostic marker.

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Suppression of Integrin α3β1 in Breast Cancer Cells Reduces Cyclooxygenase-2 Gene Expression and Inhibits Tumorigenesis, Invasion, and Cross-Talk to Endothelial Cells

Cited by 80 publications

References 48 publications

Hypoxia-induced Changes to Integrin α 3 Glycosylation Facilitate Invasion in Epidermoid Carcinoma Cell Line A431

Hypoxia-induced Changes to Integrin α 3 Glycosylation Facilitate Invasion in Epidermoid Carcinoma Cell Line A431

Integrin α3β1 controls mRNA splicing that determines cyclooxygenase-2 (Cox-2) mRNA stability in breast cancer cells

COX-2 expression correlation with invasion in human breast carcinomas and in cell line MDA-MB-231 in vitro

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