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dc.contributor.author Ligtenberg, Maarten A.
dc.contributor.author Rojas-Colonelli, Nicole
dc.contributor.author Kiessling, Rolf
dc.contributor.author Uadser, Alvaro
dc.date.accessioned 2024-09-26T00:29:22Z
dc.date.available 2024-09-26T00:29:22Z
dc.date.issued 2013-10
dc.identifier.issn 2164-5515
dc.identifier.uri https://repositorio.uss.cl/handle/uss/12321
dc.description Funding Information: Research described here have been supported by grants to AL and RK from FONDECYT 11110525, CONICYT 791100038, CONICYT Program PFB-16, CORFO-Innova 12IDL2-13348, The Swedish Medical Research Council (K2011-66X-15387-07-3 VR), The Swedish Cancer Society (12 0598
dc.description.abstract DNA vaccines have been shown to elicit tumor-protective cytotoxic T lymphocyte (CTL) immunity in preclinical models, but have shown limited efficacy in cancer patients. Plasmids used for DNA vaccines can stimulate several innate immune receptors, triggering the activation of master transcription factors, including interferon regulatory factor 3 (IRF3) and nuclear factor k B (NF-kB). These transcription factors drive the production of type I interferons (IFNs) and pro-inflammatory cytokines, which promote the induction of CTL responses. Understanding the innate immune signaling pathways triggered by DNA vaccines that control the generation of CTL responses will increase our ability to design more effective vaccines. To gain insight into the contribution of these pathways, we vaccinated mice lacking different signaling components with plasmids encoding tyrosinase-related protein 2 (TRP2) or ovalbumin (OVA) using intradermal electroporation. Antigenspecific CTL responses were detected by intracellular IFN-7 staining and in vivo cytotoxicity. Mice lacking IRF3, IFN-a receptor, IL-1 p/IL-18, TLR9 or MyD88 showed similar CTL responses to wild-type mice, arguing that none of these molecules were required for the immunogenicity of DNA vaccines. To elucidate the role of NF-kB activation we co-vaccinated mice with pkBa-SR, a plasmid encoding a mutant IκBα that blocks NF-κB activity. Mice vaccinated with plκBα-SR and the TRP2-encoding plasmid (pTRP2) drastically reduced the frequencies of TRP2-specific CTLs and were unable to suppress lung melanoma metastasis in vivo, as compared with mice vaccinated only with pTRP2. Taken together these results indicate that the activation of NF-kB is essential for the immunogenicity of intradermal DNA vaccines. en
dc.language.iso eng
dc.relation.ispartof vol. 9 Issue: no. 10 Pages: 2189-2195
dc.source Human Vaccines and Immunotherapeutics
dc.title NF-κB activation during intradermal DNA vaccination is essential for eliciting tumor protective antigen-specific CTL responses en
dc.type Artículo
dc.identifier.doi 10.4161/hv.25699
dc.publisher.department Facultad de Medicina y Ciencia


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