Profiling Bladder Cancer Organ Site-Specific Metastasis Identifies LAMC2 as a Novel Biomarker of Hematogenous Dissemination

Smith, Steven C.; Nicholson, Brandi T.; Nitz, Matthew D.; Frierson, Henry F.; Smolkin, Mark E.; El–Rifai, Wael; Theodorescu, Dan

doi:10.2353/ajpath.2009.080538

Cited by 35 publications

(42 citation statements)

References 33 publications

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“…The cutoff of 30% was used for LAMC2 positivity as in previous reports with the same antibody. 11,14,50 Vimentin was considered to be positive if ≥ 1% of cancer cells were stained in the cytoplasm as reported previously. 51,52 Detailed methods are described in the Supplementary section.…”

Section: Methodsmentioning

confidence: 99%

“…8 Besides, LAMC2 monomer expression has been frequently found in the invasive front of epithelial tumors such as ADCs of the stomach, colon, pancreas, and lung, SCCs of the esophagus, head and neck, skin and lung, and transitional cell carcinoma of the bladder. 5,[9][10][11][12][13][14] Epithelialmesenchymal transition (EMT) has a critical role in the early stages of dissemination of malignant epithelial tumors leading to metastatic spread. 15 There is growing evidence that LAMC2 expression increases in the carcinoma cells undergoing EMT, [16][17][18] and that level of LAMC2 expression is regulated directly by the EMT master regulator ZEB1 and activated β-catenin in invasive colorectal carcinoma cells.…”

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confidence: 99%

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LAMC2 enhances the metastatic potential of lung adenocarcinoma

et al. 2015

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Lung cancer is the number one cancer killer, and metastasis is the main cause of high mortality in lung cancer patients. However, mechanisms underlying the development of lung cancer metastasis remain unknown. Using genome-wide transcriptional analysis in an experimental metastasis model, we identified laminin γ2 (LAMC2), an epithelial basement membrane protein, to be significantly upregulated in lung adenocarcinoma metastatic cells. Elevated LAMC2 increased traction force, migration, and invasion of lung adenocarcinoma cells accompanied by the induction of epithelial-mesenchymal transition (EMT). LAMC2 knockdown decreased traction force, migration, and invasion accompanied by EMT reduction in vitro, and attenuated metastasis in mice. LAMC2 promoted migration and invasion via EMT that was integrin β1-and ZEB1-dependent. High LAMC2 was significantly correlated with the mesenchymal marker vimentin expression in lung adenocarcinomas, and with higher risk of recurrence or death in patients with lung adenocarcinoma. We suggest that LAMC2 promotes metastasis in lung adenocarcinoma via EMT and may be a potential therapeutic target. Cell Death and Differentiation (2015) 22, 1341-1352; doi:10.1038/cdd.2014.228; published online 16 January 2015Lung cancer is the leading cause of cancer-related death. 1 Non-small-cell lung cancer (NSCLC) accounts for~80-85% of lung cancers. 2 Only 20-30% of NSCLC are radically resectable and the majority of lung cancer patients succumb to the disease. The high mortality of NSCLC is largely attributable to late diagnosis, when metastases are present. 2 The molecular mechanisms governing metastasis of NSCLC remain poorly understood.Metastasis is a complex, multistep process, involving migration and invasion of malignant cells from the primary tumor to blood vessels, intravasation, and survival in the circulation, and ultimately extravasation, colonization, and formation of secondary tumor at distant target organs. 3 Each of these events is classically driven by the acquisition of genetic and/or epigenetic traits in tumor cells and the cooperation of nonneoplastic stromal cells. Increased or decreased expression of several genes in tumors has been found to be correlated with metastasis. 3 However, specific gene alterations that drive NSCLC metastasis remain largely elusive.Laminin γ2 (LAMC2) is a subunit of the heterotrimeric glycoprotein laminin-332 (LAM-332, formerly laminin-5), consisting of the α3, β3, and γ2 chains. Although LAMC2 is an important structural component of the epithelial basement membrane (BM) in various normal tissues, 4 there is an emerging evidence for a pathological role of LAMC2 monomer in cancer. It has been demonstrated that LAMC2 protein expression correlates with clinical outcome of stage I lung adenocarcinoma (ADC) patients. 5,6 In addition, noncontinuous expression pattern of LAMC2 predicts the prognosis of esophageal squamous cell carcinoma (SCC), 7 and secreted LAMC2 in the serum is associated with the aggressiveness of pancreatic cancer. 8 Besides, LAMC2 monom...

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Section: Methodsmentioning

confidence: 99%

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confidence: 99%

LAMC2 enhances the metastatic potential of lung adenocarcinoma

et al. 2015

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“…Bladder cancer cells (2x10 6 ) were suspended in 0.1 ml serum-free RPMI-1640 medium and injected into the tail vein of 6-to 8-week-old nude mice (BALB/cAJcI-nu/nu; Clea Japan, Inc., Tokyo, Japan). After 3 weeks, lungs were harvested and fixed with formalin.…”

Section: Cells Reagents and Antibodiesmentioning

confidence: 99%

“…In patients with aggressive bladder cancer, the most common site of hematogenous metastasis is the lungs (6). The circulating bladder cancer cells exit the lung microvessels by transendothelial invasion, to enter the lung tissue.…”

Section: Introductionmentioning

confidence: 99%

Extravasation during bladder cancer metastasis requires cortactin-mediated invadopodia formation

Tokui

Yoneyama

Hatakeyama

et al. 2014

Molecular Medicine Reports

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Abstract. Invasive cancer cells form the filamentous actin-based membrane protrusions known as invadopodia. Invadopodia are thought to play a critical role in cancer cell invasion and metastasis due to their ability to degrade the extracellular matrix. The present study assessed whether invadopodia formation is essential in extravasation of circulating bladder cancer cells and lung metastasis. To analyze the importance of invadopodia, bladder cancer cell lines with reduced invadopodia formation were established by silencing the expression of cortactin, an essential component of invadopodia, using cortactin short hairpin RNA. Bladder cancer cells with cortactin knockdown demonstrated a markedly decreased ability to form invadopodia, secrete matrix metalloproteinases and invade the extracellular matrix. In addition, the knockdown cells exhibited a reduced transendothelial invasion capacity and decreased formation of metastatic foci in the lungs. The present study demonstrated that bladder cancer cells with cortactin knockdown have a reduced capacity to extravasate into the lung from the circulation, due to the decreased invasive character of invadopodia. This suggests that invadopodia formation is a critical process for cancer cell extravasation. IntroductionThe majority of cancer mortalities are caused by metastasis. Hematogenous metastasis includes multiple steps. First, invasive cancer cells escape from the primary site into nearby blood vessels (intravasation) and disseminate around the body through the host circulation. Following this, the circulating cancer cells exit the vessels to cross the endothelia and invade secondary organ tissue (extravasation), where they proliferate to form metastases (1). It is vital to elucidate the detailed processes of these steps to prevent metastasis, however, at present, the molecular mechanisms underlying each step remain poorly understood.In order to invade surrounding tissues, invasive cancer cells form invadopodia, the filamentous actin (F-actin)-based membrane protrusions required for degradation of the extracellular matrix (ECM) and migration through the tissues (2-4). It has been reported that invadopodia play an essential role in the intravasation of cancer cells from the primary site into the blood vessels (5). However, the importance of invadopodia formation in extravasation from the blood vessels into the target organs during metastasis, remains poorly understood.In patients with aggressive bladder cancer, the most common site of hematogenous metastasis is the lungs (6). The circulating bladder cancer cells exit the lung microvessels by transendothelial invasion, to enter the lung tissue. The present study assessed whether invadopodia formation is involved in extravasation by analyzing lung metastasis of aggressive bladder cancer cells. Materials and methods Cells, reagents and antibodies.A human invasive and high-grade bladder cancer cell line, YTS-1, was provided by Dr H. Kakizaki (Yamagata University, Yamagata, Japan). YTS-1 cells were maintained in RPMI-1640 m...

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“…We performed IHC on a 142-sample TMA 35 from patients with bladder cancer who underwent cystectomy. The intensity of RREB1 staining was scored as negative, low/focal, moderate, and high ( Figure 6A).…”

Section: Rreb1 Protein Expression Does Not Predict Overall Survival Imentioning

confidence: 99%

RREB1 Transcription Factor Splice Variants in Urologic Cancer

Nitz

Harding

Smith

et al. 2011

The American Journal of Pathology

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RREB1 is an alternatively spliced transcription factor implicated in Ras signaling and cancer. Little is known about the expression of RREB1 isoforms in cell lines or human tumors, or about the clinical relevance of the latter. We have developed tools for IHC of RREB1 protein isoform-specific amplification of RREB1 mRNA and selective knockdown of RREB1 isoforms and use these to provide new information by characterizing RREB1 expression in bladder and prostate cancer cell lines and human tissue samples. Previously described splice variants RREB1␣, RREB1␤, RREB1␥, and RREB1␦ were identified, as well as the novel variant RREB1 . Total and isoform-specific mRNA expression was lower in most but not all tumors, compared with normal tissues. RREB1 IHC performed on a bladder cancer TMA did not indicate a relationship between total RREB1 expression and overall survival after radical cystectomy for invasive bladder cancer. In contrast, in vitro proliferation studies using the UMUC-3 bladder cancer cell line after selective isoform-specific knockdown of expression indicate that RREB1␣ is not necessary for proliferation, but that RREB1␤ may be required. These contributions should accelerate progress in the nascent RREB1 field by providing new reagents while also providing clues to the role of RREB1 isoforms in human cancer and raising the possibility of isoform-specific roles in human carcinogenesis and progression.

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Profiling Bladder Cancer Organ Site-Specific Metastasis Identifies LAMC2 as a Novel Biomarker of Hematogenous Dissemination

Cited by 35 publications

References 33 publications

LAMC2 enhances the metastatic potential of lung adenocarcinoma

LAMC2 enhances the metastatic potential of lung adenocarcinoma

Extravasation during bladder cancer metastasis requires cortactin-mediated invadopodia formation

RREB1 Transcription Factor Splice Variants in Urologic Cancer

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