Epithelial to mesenchymal transition (EMT) in human prostate cancer: lessons learned from ARCaP model

Zhau, Haiyen E.; Odero-Marah, Valerie; Lue, Hui-Wen; Nomura, Takeo; Wang, Ruoxiang; Chu, Gina Chia‐Yi; Liu, Zhi-Ren; Zhou, Binhua P.; Huang, Wen-Chin; Chung, Leland W.K.

doi:10.1007/s10585-008-9183-1

Cited by 134 publications

(162 citation statements)

References 40 publications

(53 reference statements)

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“…Upon exposure to certain soluble factors or host bone microenvironment, low-invasive and epithelial-like ARCaP E cells undergo EMT and acquire invasive properties (26,27). Western blot analysis showed that both EGFR and neu (HER2/ ErbB2) were highly expressed and phosphorylated in ARCaP E cells and their highly metastatic, mesenchymal-like counterparts ARCaP M cells (Fig.…”

Section: Resultsmentioning

confidence: 98%

Epidermal Growth Factor Promotes Protein Degradation of Epithelial Protein Lost in Neoplasm (EPLIN), a Putative Metastasis Suppressor, during Epithelial-mesenchymal Transition

Zhang

Wang

Iqbal

et al. 2013

Journal of Biological Chemistry

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Background:The mechanism of EGF signaling in the regulation of prostate cancer (PCa) metastasis remains unclear. Results: EGF promotes epithelial-mesenchymal transition (EMT) and induces degradation of epithelial protein lost in neoplasm (EPLIN), a putative suppressor of PCa metastasis. Conclusion: EGF activates ERK1/2-dependent phosphorylation, ubiquitination, and protein turnover of EPLIN. Significance: This study suggested that blockade of EGF signaling could retard EMT and inhibit invasiveness of PCa cells.

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Section: Resultsmentioning

confidence: 98%

Epidermal Growth Factor Promotes Protein Degradation of Epithelial Protein Lost in Neoplasm (EPLIN), a Putative Metastasis Suppressor, during Epithelial-mesenchymal Transition

Zhang

Wang

Iqbal

et al. 2013

Journal of Biological Chemistry

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“…35 Therefore, we defined by Western Blot analysis the expression profiles of the proteins involved in EMT in normal and hypoxic conditions and their variations following ANXA1 downregulation. Our results showed a significant reversion of EMT process upon ANXA1 knock down in normoxia and hypoxia exposed PCa cells suggested by noteworthy E-cadherin enhancement and vimentin decrease (Fig.…”

Section: Anxa1 Expression Strictly Correlates With Pca Cell Mesenchymmentioning

confidence: 99%

Hypoxia regulates ANXA1 expression to support prostate cancer cell invasion and aggressiveness

Bizzarro

Belvedere

Migliaro

et al. 2016

Cell Adhesion & Migration

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Annexin A1 (ANXA1) is a Ca 2C -binding protein overexpressed in the invasive stages of prostate cancer (PCa) development; however, its role in this tumor metastatization is largely unknown. Moreover, hypoxic conditions in solid tumors have been related to poor prognosis in PCa patients. We have previously demonstrated that ANXA1 is implicated in the acquisition of chemo-resistant features in DU145 PCa cells conferring them a mesenchymal/metastatic phenotype. In this study, we have investigated the mechanisms by which ANXA1 regulates metastatic behavior in LNCaP, DU145 and PC3 cells exposed to hypoxia. ANXA1 was differentially expressed by PCa cell lines in normoxia whereas hypoxic stimuli resulted in a significant increase of protein expression. Additionally, in low oxygen conditions ANXA1 was extensively secreted out-side the cells where its binding to formyl peptide receptors (FPRs) induced cell invasion. Loss and gain of function experiments performed by using the RNA interfering siANXA1 and an ANXA1 over-expressing plasmid (MF-ANXA1), also confirmed the leading role of the protein in modulating LNCaP, DU145 and PC3 cell invasiveness. Finally, ANXA1 played a crucial role in the regulation of cytoskeletal dynamics underlying metastatization process, such as the loss of adhesion molecules and the occurrence of the epithelial to mesenchymal transition (EMT). ANXA1 expression increased inversely to epithelial markers such as E-cadherin and cytokeratins 8 and 18 (CKs) and proportionally to mesenchymal ones such as vimentin, ezrin and moesin. Our results indicated that ANXA1 may be a key mediator of hypoxia-related metastasis-associated processes in PCa.

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“…Furthermore, we found that recombinant 2-m protein could phosphorylate the Bcl-xL/Bcl-2-associated death-promoting protein, Bad, at Ser136 and Ser112 via activated PI3K/Akt and ERK signaling pathways in renal carcinoma SN12C cells [33]. Using a robust human prostate cancer EMT progression model, Zhau et al [63] from our group also showed that 2-m stably transfected ARCaP E prostate cancer cells had consistently activated STAT3, Snail, LIV-1, and overexpressed LIV-1 and receptor activator of nuclear factor kappa B ligand (RANKL)…”

Section: Roles Of 2-m In Signaling Pathways In Cancer Cellsmentioning

confidence: 96%

“…Previous studies have supported the association of increased EMT with the ability of cancer cells to migrate, invade, and metastasize to the skeleton. 2-m also regulates cancer bone metastasis and confers cancer lethality through EMT by downregulation of E-cadherin and upregulation of N-cadherin, vimentin, and RANKL in solid tumors [34,63].…”

Section: Roles Of 2-m In Interaction Between Cancer Cells and Bone MImentioning

confidence: 99%

Test Article

2014

ScienceOpen Research

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2-microglobulin ( 2-m) has become the focus of intense scrutiny since the discovery of its undesirable roles promoting osteomimicry and cancer progression. 2-m is a well-known housekeeping protein that forms complexes with the heavy chain of major histocompatibility complex class I molecules, which are heterodimeric cell surface proteins that present antigenic peptides to cytotoxic T cells. On recognition of foreign peptide antigens on cell surfaces, T cells actively bind and lyse antigen-presenting cancer cells. In addition to its roles in tumor immunity, 2-m has two different functions in cancer cells, either tumor promoting or tumor suppressing, in cancer cell context-dependent manner. Our studies have demonstrated that 2-m is involved extensively in the functional regulation of growth, survival, apoptosis, and even metastasis of cancer cells. We found that 2-m is a soluble growth factor and a pleiotropic signaling molecule which interacts with its receptor, hemochromatosis protein, to modulate epithelial-to-mesenchymal transition (EMT) through iron-responsive pathways. Specific antibodies against 2-m have remarkable tumoricidal activity in cancer, through 2-m action on iron flux, alterations of intracellular reactive oxygen species, DNA damage and repair enzyme activities, -catenin activation and cadherin switching, and tumor responsiveness to hypoxia. These novel functions of 2-m and 2-m signaling may be common to several solid tumors including human lung, breast, renal, and prostate cancers. Our experimental results could lead to the development of a novel class of antibody-based pharmaceutical agents for cancer growth control. In this review, we briefly summarize the recent data regarding 2-m as a promising new cancer therapeutic target and discuss antagonizing this therapeutic target with antibody therapy for the treatment of localized and disseminated cancers.Keywords: Anti-2-m antibody, apoptosis, 2-microglobulin ( 2-m), osteomimicry. INTRODUCTION2-microglobulin ( 2-m), a well-known housekeeping gene, is a nonglycosylated protein with a low molecular weight of 12-kDa. This 99-amino acid residue protein is synthesized by all nucleated cells. It has been identified as a major structural component of amyloid fibrils deposited in dialysis-related amyloidosis, a common and serious complication in patients receiving hemodialysis for more than 10 years [1, 2]. 2-m forms a small invariable light chain subunit of the major histocompatibility complex (MHC) class I antigen, also known as human leukocyte antigen (HLA), on the cell surface of nucleated cells. 2-m is an important structural protein in the regulation of host immune recognition of self and non-self antigens by CD8 + T lymphocytes and for immunoglobulin transport and iron metabolism [3][4][5][6]. Some animal studies have reported that even when no MHC class I antigens could be detected on cells and the animals were grossly deficient in CD4 -CD8 + T cells, which normally mediate cytotoxic T cell function, the homozygotes appeared normal [7,8]....

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Epithelial to mesenchymal transition (EMT) in human prostate cancer: lessons learned from ARCaP model

Cited by 134 publications

References 40 publications

Epidermal Growth Factor Promotes Protein Degradation of Epithelial Protein Lost in Neoplasm (EPLIN), a Putative Metastasis Suppressor, during Epithelial-mesenchymal Transition

Epidermal Growth Factor Promotes Protein Degradation of Epithelial Protein Lost in Neoplasm (EPLIN), a Putative Metastasis Suppressor, during Epithelial-mesenchymal Transition

Hypoxia regulates ANXA1 expression to support prostate cancer cell invasion and aggressiveness

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