Your search keyword '"Mei-Sze Chua"' showing total 3 results

1. Blockade of Wnt-1 signaling leads to anti-tumor effects in hepatocellular carcinoma cells

Author

Samuel So, Mei-Sze Chua, Susan Grepper, and Wei Wei

Subjects

Adult, Cancer Research, Beta-catenin, Carcinoma, Hepatocellular, Cell Survival, Blotting, Western, Mice, Nude, Wnt1 Protein, medicine.disease_cause, lcsh:RC254-282, Mice, Liver Neoplasms, Experimental, Transcription Factor 4, Cell Line, Tumor, medicine, Carcinoma, Animals, Humans, Cells, Cultured, beta Catenin, Aged, Cell Proliferation, biology, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Research, Wnt signaling pathway, Antibodies, Monoclonal, Middle Aged, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immunohistochemistry, Xenograft Model Antitumor Assays, digestive system diseases, Blockade, Gene Expression Regulation, Neoplastic, Oncology, Hepatocellular carcinoma, Immunology, biology.protein, Cancer research, Hepatocytes, Experimental pathology, Molecular Medicine, Signal transduction, Carcinogenesis, Signal Transduction, Transcription Factors

Abstract

BackgroundHepatocellular carcinoma (HCC) is an aggressive cancer, and is the third leading cause of cancer death worldwide. Standard therapy is ineffective partly because HCC is intrinsically resistant to conventional chemotherapy. Its poor prognosis and limited treatment options make it critical to develop novel and selective chemotherapeutic agents. Since the Wnt/β-catenin pathway is essential in HCC carcinogenesis, we studied the inhibition of Wnt-1-mediated signaling as a potential molecular target in HCC.ResultsWe demonstrated that Wnt-1 is highly expressed in human hepatoma cell lines and a subgroup of human HCC tissues compared to paired adjacent non-tumor tissues. An anti-Wnt-1 antibody dose-dependently decreased viability and proliferation of Huh7 and Hep40 cells over-expressing Wnt-1 and harboring wild type β-catenin, but did not affect normal hepatocytes with undetectable Wnt-1 expression. Apoptosis was also observed in Huh7 and Hep40 cells after treatment with anti-Wnt-1 antibody. In these two cell lines, the anti-Wnt-1 antibody decreased β-catenin/Tcf4 transcriptional activities, which were associated with down-regulation of the endogenous β-catenin/Tcf4 target genes c-Myc, cyclin D1, and survivin. Intratumoral injection of anti-Wnt-1 antibody suppressedin vivotumor growth in a Huh7 xenograft model, which was also associated with apoptosis and reduced c-Myc, cyclin D1, and survivin expressions.ConclusionOur results suggest that Wnt-1 is a survival factor for HCC cells, and that the blockade of Wnt-1-mediated signaling may offer a potential pathway-specific therapeutic strategy for the treatment of a subgroup of HCC that over-expresses Wnt-1.

Published

2009

2. Soluble Frizzled-7 receptor inhibits Wnt signaling and sensitizes hepatocellular carcinoma cells towards doxorubicin.

Author

Wei Wei, Mei-Sze Chua, Grepper, Susan, and So, Samuel K.

Subjects

*LIVER cancer, *DOXORUBICIN, *ESCHERICHIA coli, *TRANSCRIPTION factors, *ANTHRACYCLINES

Abstract

Background: There are limited therapeutic options for hepatocellular carcinoma (HCC), the most common liver malignancy worldwide. Recent studies have identified the Frizzled-7 receptor (FZD7), important for activation of Wnt-mediated signaling, as a potential therapeutic target for HCC and other cancers. Methods: We hypothesized that the extracellular domain of FZD7 (sFZD7) would be a clinically more relevant therapeutic modality than previously studied approaches to target FZD7. We expressed and purified sFZD7 from E. coli, and tested its functional activity to interact with Wnt3, its ability to inhibit Wnt3-mediated signaling, and its potential for combinatorial therapy in HCC. Results: sFZD7 pulled down Wnt3 from Huh7 cells, and decreased β-catenin/Tcf4 transcriptional activity in HCC cells. In vitro, sFZD7 dose-dependently decreased viability of three HCC cell lines (HepG2, Hep40, and Huh7, all with high FZD7 and Wnt3 mRNA), but had little effect on normal hepatocytes from three donors (all with low level FZD7 and Wnt3 mRNA). When combined with doxorubicin, sFZD7 enhanced the growth inhibitory effects of doxorubicin against HCC cells in vitro, and against Huh7 xenografts in vivo. Reduced expressions of c-Myc, cyclin D1, and survivin were observed in vitro and in vivo. Additionally, sFZD7 altered the levels of phosphorylated AKT and ERK1/2 induced by doxorubicin treatment in vitro, suggesting that several critical pathways are involved in the chemosensitizing effect of sFZD7. Conclusions: We propose that sFZD7 is a feasible therapeutic agent with specific activity, which can potentially be combined with other chemotherapeutic agents for the improved management of HCC. [ABSTRACT FROM AUTHOR]

Published

2011

3. Small interfering RNA targeting CDC25B inhibits liver tumor growth in vitro and in vivo.

Author

Xinrui Yan, Mei-Sze Chua, Jing He, and So, Samuel K.

Subjects

*GENE expression, *PHOSPHATASES, *CANCER cell growth regulation, *LIVER cancer, *CYCLIN-dependent kinases, *CELL cycle regulation, *RNA, *LABORATORY mice

Abstract

Background: Using gene expression profiling, we previously identified CDC25B to be significantly highly expressed in hepatocellular carcinoma (HCC) compared to non-tumor liver. CDC25B is a cell cycle-activating phosphatase that positively regulates the activity of cyclin-dependent kinases, and is over-expressed in a variety of human malignancies. In this study, we validated the overexpression of CDC25B in HCC, and further investigated its potential as a therapeutic target for the management of HCC. Results: Quantitative real-time polymerase chain reaction and immunohistochemical staining of patient samples confirmed the significant over-expression of CDC25B in HCC compared to nontumor liver samples (P < 0.001). Thus, intefering with the expression and activity of CDC25B may be a potential way to intervene with HCC progression. We used RNA interference to study the biological effects of silencing CDC25B expression in HCC cell lines (Hep3B and Hep40), in order to validate its potential as a therapeutic target. Using small oligo siRNAs targeting the coding region of CDC25B, we effectively suppressed CDC25B expression by up to 90%. This was associatetd with significant reductions in cell growth rate, cell migration and invasion through the matrigel membrane, and caused significant cell cycle delay at the G2 phase. Finally, suppression of CDC25B significantly slowed the growth of Hep40 xenografts in nude mice. Conclusion: Our data provide evidence that the inhibition of CDC25B expression and activity lead to suppression of tumor cell growth and motility, and may therefore be a feasible approach in the clinical management of HCC. [ABSTRACT FROM AUTHOR]

Published

2008