4.8 Article

Stealth Immune Properties of Graphene Oxide Enabled by Surface-Bound Complement Factor H

Journal

ACS NANO
Volume 10, Issue 11, Pages 10161-10172

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acsnano.6b05409

Keywords

factor H; serum albumin; graphene oxide; protein corona; protein coating; complement activation; immunomodulation

Funding

  1. National Research Foundation of Singapore through a Competitive Research Programme grant [NRF-CRP10-2012-07]
  2. Nanyang Technological University [M4080751.070]
  3. National Science Foundation [1509794]
  4. Div Of Electrical, Commun & Cyber Sys
  5. Directorate For Engineering [1509794] Funding Source: National Science Foundation

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With mounting evidence that nanomaterials can trigger adverse innate immune responses such as complement activation, there is increasing attention to the development of strategies that mask the complement activating properties of nanomaterials. The current gold standard to reduce complement activation of nanomaterials is the covalent attachment of polymer coatings on nanomaterial surfaces, even though this strategy provides only moderate protection against complement activation. Akin to protein coronas that form on nanomaterial surfaces in physiological fluids, noncovalent strategies based on protein adsorption would offer a simplified, biomimetic approach to mitigate complement activation. Herein, we demonstrate that precoating graphene-based nanomaterials with purified, natural proteins enables regulatory control of nanomaterial-triggered complement activation. When the graphene-based nanomaterials were coated with complement factor H, nearly complete protection (>90% reduction) against complement activation (a stealth effect) was achieved. By contrast, coating the nanomaterials with a passivating layer of bovine or human serum albumins achieved moderate protection (similar to 40% reduction), whereas immunoglobulin G amplified complement activation by several-fold. Taken together, our results demonstrate that surface-bound factor H, as well as serum albumins, can prevent graphene oxide triggered complement activation, thereby offering a facile approach to inhibit complement activation completely down to naturally occurring levels.

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