Characterization of the bionano interface and mapping extrinsic interactions of the corona of nanomaterialsElectronic supplementary information (ESI) available. See DOI: 10.1039/c5nr01970b

Nanoparticles in physiological environments are known to selectively adsorb proteins and other biomolecules forming a tightly bound biomolecular 'corona' on their surface. Where the exchange times of the proteins are sufficiently long, it is believed that the protein corona constitutes the...

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Bibliographic Details
Main Authors: O'Connell, D. J, Bombelli, F. Baldelli, Pitek, A. S, Monopoli, M. P, Cahill, D. J, Dawson, K. A
Format: Article
Language:English
Online Access:Get full text
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Summary:Nanoparticles in physiological environments are known to selectively adsorb proteins and other biomolecules forming a tightly bound biomolecular 'corona' on their surface. Where the exchange times of the proteins are sufficiently long, it is believed that the protein corona constitutes the particle identity in biological milieu. Here we show that proteins in the corona retain their functional characteristics and can specifically bind to cognate proteins on arrays of thousands of immobilised human proteins. The biological identity of the nanomaterial is seen to be specific to the blood plasma concentration in which they are exposed. We show that the resulting in situ nanoparticle interactome is dependent on the protein concentration in plasma, with the emergence of a small number of dominant protein-protein interactions. These interactions are those driven by proteins that are adsorbed onto the particle surface and whose binding epitopes are subsequently expressed or presented suitably on the particle surface. We suggest that, since specific tailored protein arrays for target systems and organs can be designed, their use may be an important element in an overall study of the biomolecular corona. Nanoparticle biomolecular corona leads the interactions with cognate proteins on arrays of thousands of immobilised human proteins.
ISSN:2040-3364
2040-3372
DOI:10.1039/c5nr01970b