4.8 Article

Graphene Nanoflake Uptake Mediated by Scavenger Receptors

Journal

NANO LETTERS
Volume 19, Issue 2, Pages 1260-1268

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.nanolett.8b04820

Keywords

Graphene; protein corona; scavenger receptors; nanobiological interactions

Funding

  1. European Union Seventh Framework Programme Graphene Flagship [604391, 696656]
  2. Irish Research Council [GOIPD/2016/128]
  3. Irish Research Council under the Enterprise Partnership PostDoctoral Fellowship Scheme [EPSPD/2015/37]
  4. EU H2020 Nanofacturing project [646364]
  5. Science Foundation Ireland (SFI) Principal Investigator Award [12/IA/1422]
  6. Science Foundation Ireland (SFI) [PI/11/08]
  7. Irish Research Council (IRC) [GOIPD/2016/128] Funding Source: Irish Research Council (IRC)

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The biological interactions of graphene have been extensively investigated over the last 10 years. However, very little is known about graphene interactions with the cell surface and how the graphene internalization process is driven and mediated by specific recognition sites at the interface with the cell. In this work, we propose a methodology to investigate direct molecular correlations between the biomolecular corona of graphene and specific cell receptors, showing that key protein recognition motifs, presented on the nanomaterial surface, can engage selectively with specific cell receptors. We consider the case of apolipoprotein A-I, found to be very abundant in the graphene protein corona, and observe that the uptake of graphene nanoflakes is somewhat increased in cells with greatly elevated expression of scavenger receptors B1, suggesting a possible mechanism of endogenous interaction. The uptake results, obtained by flow cytometry, have been confirmed using Raman microspectroscopic mapping, exploiting the strong Raman signature of graphene.

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