Journal
ACS NANO
Volume 9, Issue 2, Pages 2157-2166Publisher
AMER CHEMICAL SOC
DOI: 10.1021/nn506060q
Keywords
nanoparticle; glycosylation; protein corona; macrophage; adhesion; internalization
Categories
Funding
- European Union's Seventh Framework Programme (EU FP7) [309329]
- EU FP7 program HighGlycan [278535]
- SFI PI Award [12/IA/1422]
- Irish Research Council under the EMBARK scheme [RS/2011/106]
- Australian Research Council under the Australian Laureate Fellowship [FL120100030]
- Discovery Early Career Researcher Award [DE130100488]
- Australian Research Council Centre of Excellence in Convergent Bio-Nano Science and Technology [CE140100036]
- University of Melbourne under the Dyason Fellowship
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The significance of a protein corona on nanoparticles in modulating particle properties and their biological interactions has been widely acknowledged. The protein corona is derived from proteins in biological fluids, many of which are glycosylated. To date, the glycans on the proteins have been largely overlooked in studies of nanoparticlecell interactions. In this study, we demonstrate that glycosylation of the protein corona plays an important role in maintaining the colloidal stability of nanoparticles and influences nanoparticlecell interactions. The removal of glycans from the protein corona enhances cell membrane adhesion and cell uptake of nanoparticles in comparison with the fully glycosylated form, resulting in the generation of a pro-inflammatory milieu by macrophages. This study highlights that the post-translational modification of proteins can significantly impact nanoparticlecell interactions by modulating the protein corona properties.
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