Proteomic and Post-Translational Modification Profiling of Exosome-Mimetic Nanovesicles Compared to Exosomes

Amirmohammad Nasiri Kenari, Kenneth Kastaniegaard, David W Greening, Mitch Shambrook, Allan Stensballe, Lesley Cheng, Andrew F Hill

Research output: Contribution to journalJournal articleResearchpeer-review

52 Citations (Scopus)
264 Downloads (Pure)

Abstract

Issues associated with upscaling exosome production for therapeutic use may be overcome through utilizing artificial exosomes. Cell-derived mimetic nanovesicles (M-NVs) are a potentially promising alternative to exosomes for clinical applicability, demonstrating higher yield without incumbent production and isolation issues. Although several studies have shown that M-NVs have similar morphology, size and therapeutic potential compared to exosomes, comprehensive characterization and to what extent M-NVs components mimic exosomes remain elusive. M-NVs were generated through the extrusion of cells and proteomic profiling demonstrated an enrichment of proteins associated with membrane and cytosolic components. The proteomic data herein reveal a subset of proteins that are highly abundant in M-NVs in comparison to exosomes. M-NVs contain proteins that largely represent the parental cell proteome, whereas the profile of exosomal proteins highlight their endosomally derived origin. This advantage of M-NVs alleviates the necessity of endosomal sorting of endogenous therapeutic proteins or RNA into exosomes. This study also highlights differences in protein post-translational modifications among M-NVs, as distinct from exosomes. Overall this study provides key insights into defining the proteome composition of M-NVs as a distinct from exosomes, and the potential advantage of M-NVs as an alternative nanocarrier when spontaneous endosomal sorting of therapeutics are limited.

Original languageEnglish
Article number1800161
JournalProteomics
Volume19
Issue number8
Number of pages20
ISSN1615-9853
DOIs
Publication statusPublished - Apr 2019

Bibliographical note

© 2019 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.

Keywords

  • artificial extracellular vesicles
  • exosomes
  • extracellular vesicles
  • mimetic-nanovesicles
  • post-translational modification
  • proteomics
  • therapeutic exosomes

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