Exosomes As Potent Cell-Free Peptide-Based Vaccine. II. Exosomes in CpG Adjuvants Efficiently Prime Naive Tc1 Lymphocytes Leading to Tumor Rejection

  • Nathalie Chaput
  • , Nöel E.C. Schartz
  • , Fabrice André
  • , Julien Taïeb
  • , Sophie Novault
  • , Pierre Bonnaventure
  • , Nathalie Aubert
  • , Jacky Bernard
  • , François Lemonnier
  • , Miriam Merad
  • , Gosse Adema
  • , Malcolm Adams
  • , Maria Ferrantini
  • , Antoine F. Carpentier
  • , Bernard Escudier
  • , Thomas Tursz
  • , Eric Angevin
  • , Laurence Zitvogel

Research output: Contribution to journalArticlepeer-review

240 Scopus citations

Abstract

Ideal vaccines should be stable, safe, molecularly defined, and out-of-shelf reagents efficient at triggering effector and memory Ag-specific T cell-based immune responses. Dendritic cell-derived exosomes could be considered as novel peptide-based vaccines because exosomes harbor a discrete set of proteins, bear functional MHC class I and II molecules that can be loaded with synthetic peptides of choice, and are stable reagents that were safely used in pioneering phase I studies. However, we showed in part I that exosomes are efficient to promote primary MHC class I-restricted effector CD8+ T cell responses only when transferred onto mature DC in vivo. In this work, we bring evidence that among the clinically available reagents, Toll-like receptor 3 and 9 ligands are elective adjuvants capable of triggering efficient MHC-restricted CD8+ T cell responses when combined to exosomes. Exosome immunogenicity across species allowed to verify the efficacy of good manufactory procedures-manufactured human exosomes admixed with CpG oligonucleotides in prophylactic and therapeutic settings of melanoma in HLA-A2 transgenic mice. CpG adjuvants appear to be ideal adjuvants for exosome-based cancer vaccines.

Original languageEnglish
Pages (from-to)2137-2146
Number of pages10
JournalJournal of Immunology
Volume172
Issue number4
DOIs
StatePublished - 15 Feb 2004
Externally publishedYes

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