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PEGylated graphene oxide elicits strong immunological responses despite surface passivation

  • Nana Luo
  • , Jeffrey K. Weber
  • , Shuang Wang
  • , Binquan Luan
  • , Hua Yue
  • , Xiaobo Xi
  • , Jing Du
  • , Zaixing Yang
  • , Wei Wei*
  • , Ruhong Zhou
  • , Guanghui Ma
  • *Corresponding author for this work
  • CAS - Institute of Process Engineering
  • University of Chinese Academy of Sciences
  • IBM
  • Tsinghua University
  • Soochow University
  • Columbia University
  • Nanjing Tech University

Research output: Contribution to journalArticlepeer-review

Abstract

Engineered nanomaterials promise to transform medicine at the bio-nano interface. However, it is important to elucidate how synthetic nanomaterials interact with critical biological systems before such products can be safely utilized in humans. Past evidence suggests that polyethylene glycol-functionalized (PEGylated) nanomaterials are largely biocompatible and elicit less dramatic immune responses than their pristine counterparts. We here report results that contradict these findings. We find that PEGylated graphene oxide nanosheets (nGO-PEGs) stimulate potent cytokine responses in peritoneal macrophages, despite not being internalized. Atomistic molecular dynamics simulations support a mechanism by which nGO-PEGs preferentially adsorb onto and/or partially insert into cell membranes, thereby amplifying interactions with stimulatory surface receptors. Further experiments demonstrate that nGO-PEG indeed provokes cytokine secretion by enhancing integrin β 8 -related signalling pathways. The present results inform that surface passivation does not always prevent immunological reactions to 2D nanomaterials but also suggest applications for PEGylated nanomaterials wherein immune stimulation is desired.

Original languageEnglish
Article number14537
JournalNature Communications
Volume8
DOIs
StatePublished - 24 Feb 2017
Externally publishedYes

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