| Literature DB >> 23735821 |
Martin Schäffler1, Manuela Semmler-Behnke, Hakan Sarioglu, Shinji Takenaka, Alexander Wenk, Carsten Schleh, Stefanie M Hauck, Blair D Johnston, Wolfgang G Kreyling.
Abstract
When nanoparticles (NP) enter the body they come into contact with body fluids containing proteins which can adsorb to their surface. These proteins may influence the NP interactions with the biological vicinity, eventually determining their biological fate inside the body. Adsorption of the most abundantly binding proteins was studied after an in vitro 24 hr incubation of monodisperse, negatively charged 5, 15 and 80 nm gold spheres (AuNP) in mouse serum by a two-step analysis: proteomic protein identification and quantitative protein biochemistry. The adsorbed proteins were separated from non-adsorbed proteins by centrifugation and gel electrophoresis and identified using a MALDI-TOF-MS-Proteomics-Analyzer. Quantitative analysis of proteins in gel bands by protein densitometry, required the focus on predominantly binding serum proteins. Numerous proteins adsorbed to the AuNP depending on their size, e.g., apolipoproteins or complement C3. The qualitative and quantitative amount of adsorbed proteins differed between 5, 15 and 80 nm AuNP. Band intensities of adsorbed proteins decreased with increasing AuNP sizes based not only on their mass but also on their surface area. Summarizing, the AuNP surface is covered with serum proteins containing transport and immune related proteins among others. Hence, protein binding depends on the size, surface area and curvature of the AuNP.Entities:
Mesh:
Substances:
Year: 2013 PMID: 23735821 DOI: 10.1088/0957-4484/24/26/265103
Source DB: PubMed Journal: Nanotechnology ISSN: 0957-4484 Impact factor: 3.874