HLA-B and cysteinylated ligands distinguish the antigen presentation landscape of extracellular vesicles

Publication date

2021-12

Authors

Bauzá-Martinez, JuliaISNI 0000000492835899
Heck, AlbertORCID 0000-0002-2405-4404ISNI 0000000393921118
Wu, WeiISNI 0000000107490485

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Article
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Abstract

Extracellular vesicles can modulate diverse processes ranging from proliferation and tissue repair, to chemo-resistance and cellular differentiation. With the advent of tissue and immunological targeting, extracellular vesicles are also increasingly viewed as promising vectors to deliver peptide-based cancer antigens to the human immune system. Despite the clinical relevance and therapeutic potential of such 'cell-free' approaches, the natural antigen presentation landscape exported in extracellular vesicles is still largely uncharted, due to the challenging nature of such preparations and analyses. In the context of therapeutic vesicle production, a critical evaluation of the similarity in vesicular antigen presentation is also urgently needed. In this work, we compared the HLA-I peptide ligandomes of extracellular vesicles against that of whole-cells of the same cell line. We found that extracellular vesicles not only over-represent HLA-B complexes and peptide ligands, but also cysteinylated peptides that may modulate immune responses. Collectively, these findings describe the pre-existing provision of vesicular HLA complexes that may be utilized to carry peptide vaccines, as well as the propensity for different peptide and post-translationally modified ligands to be presented, and will outline critical considerations in devising novel EV vaccination strategies.

Keywords

Medicine (miscellaneous), General Biochemistry,Genetics and Molecular Biology, General Agricultural and Biological Sciences, SDG 3 - Good Health and Well-being

Citation

Bauzá-Martinez, J, Heck, A J R & Wu, W 2021, 'HLA-B and cysteinylated ligands distinguish the antigen presentation landscape of extracellular vesicles', Communications Biology, vol. 4, no. 1, 825, pp. 1-11. https://doi.org/10.1038/s42003-021-02364-y