AI Article Synopsis
- Beta-catenin is often overexpressed in various cancers, including esophageal cancer, and contributes to tumor growth and cell proliferation.
- Researchers silenced beta-catenin in a specific esophageal cancer cell line using a DNA template to trigger RNA interference, which resulted in reduced beta-catenin expression and inhibited tumor cell growth.
- The study found that lowering beta-catenin led to cell cycle arrest without cell death and significantly reduced tumor growth in animal models, suggesting this method could be a new treatment approach for esophageal cancer.
Article Abstract
beta-Catenin, which is frequently overexpressed in a variety of human cancers including esophageal cancer, mediates cancer cell proliferation and tumor growth. In the present study, we used a human U6 promoter-driven DNA-template approach to induce short hairpin RNA (shRNA)-triggered RNA interference to silence beta-catenin gene expression in human esophageal squamous cell carcinoma cell line Eca-109, and then evaluated its effects on the proliferation and growth of tumor cells in vitro and in nude mice. beta-Catenin expression levels decreased markedly in Eca-109 cells transfected with a plasmid expressing shRNA for beta-catenin. Downregulation of beta-catenin was concomitantly accompanied by reduction of cyclin D1, colony formation, and growth inhibition of Eca-109 cells in vitro. The mechanism appears to be the G0/G1 phase arrest but not induction of apoptosis. In vivo, treatment of Eca-109 cells with beta-catenin shRNA greatly impeded tumor growth in nude mice. We conclude that plasmid vector-mediated beta-catenin RNA interference holds great promise as a novel treatment on human esophageal cancer with beta-catenin overexpression.
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| http://dx.doi.org/10.1111/j.1442-2050.2008.00875.x | DOI Listing |
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