Enrichment of immunoregulatory proteins in the biomolecular corona of nanoparticles within human respiratory tract lining fluid

  • Abhinav Kumar
  • , Elif Melis Bicer
  • , Anna Babin Morgan
  • , Paul E. Pfeffer
  • , Marco Monopoli
  • , Kenneth A. Dawson
  • , Jonny Eriksson
  • , Katarina Edwards
  • , Steven Lynham
  • , Matthew Arno
  • , Annelie F. Behndig
  • , Anders Blomberg
  • , Graham Somers
  • , Dave Hassall
  • , Lea Ann Dailey
  • , Ben Forbes
  • , Ian S. Mudway

    Research output: Contribution to journalArticlepeer-review

    Abstract

    When inhaled nanoparticles deposit in the lungs, they transit through respiratory tract lining fluid (RTLF) acquiring a biomolecular corona reflecting the interaction of the RTLF with the nanomaterial surface. Label-free snapshot proteomics was used to generate semi-quantitative profiles of corona proteins formed around silica (SiO2) and poly(vinyl) acetate (PVAc) nanoparticles in RTLF, the latter employed as an archetype drug delivery vehicle. The evolved PVAc corona was significantly enriched compared to that observed on SiO2 nanoparticles (698 vs. 429 proteins identified); however both coronas contained a substantial contribution from innate immunity proteins, including surfactant protein A, napsin A and complement (C1q and C3) proteins. Functional protein classification supports the hypothesis that corona formation in RTLF constitutes opsonisation, preparing particles for phagocytosis and clearance from the lungs. These data highlight how an understanding of the evolved corona is necessary for the design of inhaled nanomedicines with acceptable safety and tailored clearance profiles.
    Original languageEnglish
    Pages (from-to)1033-1043
    JournalJournal of Smooth Muscle Research
    Volume12
    Issue number4
    Early online date6 Jan 2016
    DOIs
    Publication statusPublished - 31 May 2016

    Keywords

    • Biological sciences

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