Listeria monocytogenes can be used to deliver protein antigens or DNA and mRNA encoding such antigens directly into the cytosol of host cells because of its intracellular lifestyle. In this study, we compare the in vivo efficiencies of activation of antigen-specific CD8 and CD4 T cells when the antigen is secreted by L. monocytogenes or when antigen-encoding plasmid DNA or mRNA is released by self-destructing strains of L. monocytogenes. Infection of mice with self-destructing L. monocytogenes carriers delivering mRNA that encodes a nonsecreted form of ovalbumin (OVA) resulted in a significant OVA-specific CD8 T-cell response. In contrast, infection with L. monocytogenes delivering OVA-encoding DNA failed to generate specific T cells. Secretion of OVA by the carrier bacteria yielded the strongest immune response involving OVA-specific CD8 and CD4 T cells. In addition, we investigated the antigen delivery capacity of a self-destructing, virulence-attenuated L. monocytogenes aroA/B mutant. In contrast to the wild-type strain, this mutant exhibited only marginal liver toxicity when high doses (5 ؋ 10 7 CFU per animal administered intravenously) were used, and it was also able to deliver sufficient amounts of secreted OVA into mice. Therefore, the results presented here could lay the groundwork for a rational combination of L. monocytogenes as an attenuated carrier for the delivery of protein and nucleic acid vaccines in novel vaccination strategies.The use of virulence-attenuated bacteria as carriers for heterologous protein antigens is a versatile vaccination approach (for a review see reference 15). Bacteria directly target vaccine antigens to the appropriate cells of the immune system, such as dendritic cells (DC), for antigen presentation (17), and they act as strong immune potentiators due to their naturally produced bacterial components (pathogen-associated molecular patterns) that stimulate and modulate early innate immune responses, encouraging the generation of robust and long-lasting adaptive immune responses (11).In the majority of cases so far, virulence-attenuated strains of enteric bacterial pathogens like Salmonella, Shigella, Yersinia, Vibrio, Escherichia coli, or Listeria have been used for vaccine delivery (15). These bacteria, which can be inoculated orally, are able to cross the intestinal mucosa and induce systemic immunity as well as mucosal immunity. Therefore, virulence-attenuated bacteria are optimal candidates as carriers for heterologous protein antigens, antigen-encoding DNA (DNA vaccines), and other molecules for vaccination or other therapeutic purposes (15).In particular, the bacteria that are able to replicate and release antigen within the cytosol of eukaryotic host cells are attractive candidates for the elicitation of cell-mediated immunity against heterologous antigens. Listeria monocytogenes, a gram-positive bacterium, has been used successfully in several studies performed with different animal models to deliver tumor, viral, or parasite antigens, as well as different cytokines...
