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. 2007 Dec 3;55(6):387. doi: 10.1007/s00005-007-0044-4

DNA vaccines: are they still just a powerful tool for the future?

Jana Běláková 1,, Milada Horynová 1, Michal Křupka 1, Evžen Weigl 1, Milan Raška 1
PMCID: PMC7079751  PMID: 18060369

Abstract

Vaccination is historically one of the most successful strategies for the prevention of infectious diseases. For safety reasons, modern vaccinology tends toward the usage of inactivated or attenuated microorganisms and uses predominantly subunit vaccines. The antigens need to be clearly defined, pure, stable, appropriately composed, and properly presented to the immune system of the host. Differing ratios of various proportions between specific CD4+ and CD8+ T cell responses are essential for conferring the required protection in the case of individual vaccines. To stimulate both CD4+ and CD8+ T cells, the antigens must be processed and presented to both antigen-presentation pathways, MHC I and MHC II. Protein antigens delivered by vaccination are processed as extracellular antigens. However, extracellularly delivered antigen can be directed towards intracellular presentation pathways in conjugation with molecules involved in antigen cross-presentation, e.g. heat shock proteins, or by genomic-DNA vaccination. In this overview, current knowledge of the host immune response to DNA vaccines is summarized in the introduction. The subsequent sections discuss techniques for enhancing DNA vaccine efficacy, such as DNA delivery to specific tissues, delivery of DNA to the cell cytoplasm or nucleus, and enhancement of the immune response using molecular adjuvants. Finally, the prospects of DNA vaccination and ongoing clinical trials with various DNA vaccines are discussed.

Keywords: DNA vaccine, plasmid, delivery systems, CTL, MHC I, MHC II


Articles from Archivum Immunologiae et Therapiae Experimentalis are provided here courtesy of Nature Publishing Group

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