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Exosomal cancer immunotherapy is independent of MHC molecules on exosomes.


ABSTRACT: Peptide-loaded exosomes are promising cancer treatment vehicles; however, moderate T cell responses in human clinical trials indicate a need to further understand exosome-induced immunity. We previously demonstrated that antigen-loaded exosomes carry whole protein antigens and require B cells for inducing antigen-specific T cells. Therefore, we investigated the relative importance of exosomal major histocompatibility complex (MHC) class I for the induction of antigen-specific T cell responses and tumour protection. We show that ovalbumin-loaded dendritic cell-derived exosomes from MHCI-/- mice induce antigen-specific T cells at the same magnitude as wild type exosomes. Furthermore, exosomes lacking MHC class I, as well as exosomes with both MHC class I and II mismatch, induced tumour infiltrating T cells and increased overall survival to the same extent as syngeneic exosomes in B16 melanoma. In conclusion, T cell responses are independent of exosomal MHC/peptide complexes if whole antigen is present. This establishes the prospective of using impersonalised exosomes, and will greatly increase the feasibility of designing exosome-based vaccines or therapeutic approaches in humans.

SUBMITTER: Hiltbrunner S 

PROVIDER: S-EPMC5122422 | biostudies-literature | 2016 Jun

REPOSITORIES: biostudies-literature

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Exosomal cancer immunotherapy is independent of MHC molecules on exosomes.

Hiltbrunner Stefanie S   Larssen Pia P   Eldh Maria M   Martinez-Bravo Maria-Jose MJ   Wagner Arnika K AK   Karlsson Mikael C I MC   Gabrielsson Susanne S  

Oncotarget 20160601 25


Peptide-loaded exosomes are promising cancer treatment vehicles; however, moderate T cell responses in human clinical trials indicate a need to further understand exosome-induced immunity. We previously demonstrated that antigen-loaded exosomes carry whole protein antigens and require B cells for inducing antigen-specific T cells. Therefore, we investigated the relative importance of exosomal major histocompatibility complex (MHC) class I for the induction of antigen-specific T cell responses an  ...[more]

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2016-09-27 | PXD001808 | Pride