4.5 Article

Therapeutic vaccination with Salmonella-delivered codon-optimized outer inflammatory protein DNA vaccine enhances protection in Helicobacter pylori infected mice

期刊

VACCINE
卷 30, 期 36, 页码 5310-5315

出版社

ELSEVIER SCI LTD
DOI: 10.1016/j.vaccine.2012.06.052

关键词

Attenuated Salmonella typhimurium; Codon-optimization; Helicobacter pylori; Outer inflammatory protein; Vaccine

资金

  1. Key Sci-Tech Research Foundation of Fujian Province of China [2009Y0024]
  2. Natural Science Foundation of Fujian Province of China [2009J01145]
  3. Research Foundation of Education Bureau of Fujian Province [JA08098]
  4. Key Program of Scientific Research of Fujian Medical University of China [09ZD018]

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Vaccination had demonstrated as an alternative way to combat Helicobacter pylori challenge. In the present study, codon-optimized outer inflammatory protein gene (oipA) for Mus species codon usage, the inclusion of optimal Kozak sequence, and modified of GC content was applied to construct a novel DNA construct. The Salmonella-delivered wild type oipA construct (SL7207/poipA) and the Salmonella-delivered codon-optimized oipA construct (SL7207/poipA-opt) were prepared and their therapeutic efficacy was evaluated in H. pylori-infected mice. The codon-optimized oipA construct (poipA-opt) expressed almost six-fold higher protein than that of wild type construct (poipA) as normalized to the beta-actin expression in AGS cells. Oral therapeutic immunization with SL7207/poipA-opt significantly eliminated H. pylori colonization in the stomach; and protection was related to a robust Th1/Th2 immune response. Therefore, our results suggested that fine therapeutic efficacy was related to sufficient expression of the antigen. It is supposed that codon-optimized oipA gene improves protein expression and consequently enhances the immunogenicity of DNA vaccine, which resulted in a significant reduction of bacterial loads in H. pylori infected mice. The Salmonella-delivered codon-optimized DNA construct could be a candidate vaccine against H. pylori for the clinical application. (c) 2012 Elsevier Ltd. All rights reserved.

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