Journal
CANCER LETTERS
Volume 263, Issue 1, Pages 67-76Publisher
ELSEVIER IRELAND LTD
DOI: 10.1016/j.canlet.2007.12.022
Keywords
tumor vaccine; Salmonella; type III secretion system (TTSS); hepatitis B virus x gene (HBx); anti-tumor immunity
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Live attenuated bacteria have great potential for use in vaccine development due to several unique advantages, including stable antigen expression, effective antigen presentation, convenient and inexpensive delivery, and low cost of vaccine production. In this study, we expressed hepatitis B virus x gene (HBx) on mouse melanoma cells as the target antigen and constructed Salmonella-based HBx vaccines by two strategies, i.e., recombinant eukaryotic plasmid encoding HBx and a recombinant prokaryotic plasmid encoding Type III secretion system effector-HBx fusion protein. Both HBx constructs elicited significant levels of CTL reaction and IFN-gamma secreting T cells. When mice were challenged with melanoma cells expressing HBx, tumor growth rates in immunized animals were significantly slower than controls. Tumor sizes and tumor weight indices of immunized mice were also significantly lower than controls. We conclude that both strategies described in this study may lead to novel approaches of tumor vaccines. (C) 2007 Elsevier Ireland Ltd. All rights reserved.
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