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EMBO Molecular Medicine
Antigen delivery by filamentous bacteriophage fd displaying an anti‐DEC‐205 single‐chain variable fragment confers adjuvanticity by triggering a TLR9‐mediated immune response
Rossella Sartorius1  Luciana D'Apice1  Maria Trovato1  Fausta Cuccaro1  Valerio Costa2  Maria Giovanna De Leo4  Vincenzo Manuel Marzullo1  Carmelo Biondo3  Sabato D'Auria1  Maria Antonietta De Matteis4  Alfredo Ciccodicola2 
[1] Institute of Protein Biochemistry, National Council of Research, Naples, Italy;Institute of Genetics and Biophysics A. Buzzati-Traverso, National Council of Research, Naples, Italy;Department of Pediatric, Gynecological, Microbiological and Biomedical Sciences, University of Messina, Messina, Italy;Telethon Institute of Genetics and Medicine, Pozzuoli (NA), Italy
关键词: antigen delivery;    DEC‐205;    dendritic cells;    filamentous bacteriophage;    TLR9;   
DOI  :  10.15252/emmm.201404525
来源: Wiley
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【 摘 要 】

Abstract

Filamentous bacteriophage fd particles delivering antigenic determinants via DEC-205 (fdsc-αDEC) represent a powerful delivery system that induces CD8+ T-cell responses even when administered in the absence of adjuvants or maturation stimuli for dendritic cells. In order to investigate the mechanisms of this activity, RNA-Sequencing of fd-pulsed dendritic cells was performed. A significant differential expression of genes involved in innate immunity, co-stimulation and cytokine production was observed. In agreement with these findings, we demonstrate that induction of proinflammatory cytokines and type I interferon by fdsc-αDEC was MYD88 mediated and TLR9 dependent. We also found that fdsc-αDEC is delivered into LAMP-1-positive compartments and co-localizes with TLR9. Thus, phage particles containing a single-strand DNA genome rich in CpG motifs delivered via DEC-205 are able to intercept and trigger the active TLR9 innate immune receptor into late endosome/lysosomes and to enhance the immunogenicity of the displayed antigenic determinants. These findings make fd bacteriophage a valuable tool for immunization without administering exogenous adjuvants.

Synopsis

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Filamentous fd bacteriophages engineered to display antigens and targeted to dendritic cells via DEC-205 activate both innate and adaptive immune responses and are an attractive immunization system avoiding administration of exogenous adjuvants.

  • Antigens displayed on anti-DEC-205-targeted bacteriophages are efficiently cross-presented by DCs.
  • fd virions targeted to DCs via DEC-205 are delivered to endolysosomal compartments where they co-localize with active TLR9.
  • Transcriptome analysis using RNA-Seq of bacteriophage-pulsed DCs elucidates the signature induced by fd anti-DEC-205-based vaccine and showed the up-regulation of gene pathways involved in the innate and adaptive immune responses.
  • Production of pro-inflammatory cytokines and type I interferon is induced in DC-targeted bacteriophage fd particles displaying anti-DEC-205 scFv and abolished in MyD88−/− and Tlr9−/− mice.
  • fdsc-αDEC bacteriophages combine adjuvanticity and ability to activate specific immune responses, and may thus represent a relevant option in vaccinology.

【 授权许可】

CC BY   
© 2015 The Authors. Published under the terms of the CC BY 4.0 license

Creative Commons Attribution 4.0 License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

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