Nanomaterials (Feb 2020)

Surface Chemistry-Dependent Evolution of the Nanomaterial Corona on TiO<sub>2</sub> Nanomaterials Following Uptake and Sub-Cellular Localization

  • Abdullah O. Khan,
  • Alessandro Di Maio,
  • Emily J. Guggenheim,
  • Andrew J. Chetwynd,
  • Dan Pencross,
  • Selina Tang,
  • Marie-France A. Belinga-Desaunay,
  • Steven G. Thomas,
  • Joshua Z. Rappoport,
  • Iseult Lynch

DOI
https://doi.org/10.3390/nano10030401
Journal volume & issue
Vol. 10, no. 3
p. 401

Abstract

Read online

Nanomaterial (NM) surface chemistry has an established and significant effect on interactions at the nano-bio interface, with important toxicological consequences for manufactured NMs, as well as potent effects on the pharmacokinetics and efficacy of nano-therapies. In this work, the effects of different surface modifications (PVP, Dispex AA4040, and Pluronic F127) on the uptake, cellular distribution, and degradation of titanium dioxide NMs (TiO2 NMs, ~10 nm core size) are assessed and correlated with the localization of fluorescently-labeled serum proteins forming their coronas. Imaging approaches with an increasing spatial resolution, including automated high throughput live cell imaging, correlative confocal fluorescence and reflectance microscopy, and dSTORM super-resolution microscopy, are used to explore the cellular fate of these NMs and their associated serum proteins. Uncoated TiO2 NMs demonstrate a rapid loss of corona proteins, while surface coating results in the retention of the corona signal after internalization for at least 24 h (varying with coating composition). Imaging with two-color super-resolution dSTORM revealed that the apparent TiO2 NM single agglomerates observed in diffraction-limited confocal microscopy are actually adjacent smaller agglomerates, and provides novel insights into the spatial arrangement of the initial and exchanged coronas adsorbed at the NM surfaces.

Keywords