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Protein-nanoparticle interactions: Opportunities and challenges
Mahmoudi, M ; Sharif University of Technology | 2011
1517
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- Type of Document: Article
- DOI: 10.1021/cr100440g
- Publisher: 2011
- Abstract:
- The significant role of protein nanoparticle interactions in nanomedicine and nanotoxicity is emerging recently through the identification of the nanoparticles (NP) protein (biomolecule) corona. The dynamic layer of proteins and/or other biomolecules adsorbed to the nanoparticle surface determines how a NP interacts with living systems and thereby modifies the cellular responses to the NP. Ehrenberg and co-workers used cultured endothelium cells as a model for vascular transport of polystyrene NP with various functional groups, which showed that the capacity of the various NP surfaces to adsorb proteins was indicative of their tendency to associate with cells. The quantification of the adsorbed proteins showed that high-binding NP were maximally coated within seconds to minutes, indicating that proteins on the surface of NP could mediate cell association over much longer time scales. The adsorption or covalent binding of a protein onto a NP's surface can strongly alter the physio-chemical and structural properties of both of them
- Keywords:
- Cellular response ; Covalent binding ; Living systems ; Nanoparticle interaction ; Nanoparticle surface ; Physio-chemical ; Time-scales ; Vascular transport ; Adsorption ; Biomolecules ; Cells ; Functional groups ; Medical nanotechnology ; Nanoparticles ; Polystyrenes ; Chemical phenomena ; Chemistry ; Infrared spectroscopy ; Metabolism ; Methodology ; Raman spectrometry ; Review ; X ray crystallography ; Calorimetry ; Circular Dichroism ; Crystallography, X-Ray ; Electrophoresis ; Hydrophobic and Hydrophilic Interactions ; Mass Spectrometry ; Particle Size ; Protein Conformation ; Proteins ; Spectroscopy, Fourier Transform Infrared ; Spectrum Analysis, Raman ; Surface Plasmon Resonance ; Surface Properties
- Source: Chemical Reviews ; Volume 111, Issue 9 , June , 2011 , Pages 5610-5637 ; 00092665 (ISSN)
- URL: http://pubs.acs.org/doi/abs/10.1021/cr100440g