| Literature DB >> 30721573 |
I-Lun Hsiao1,2, Susanne Fritsch-Decker1, Arnold Leidner3, Marco Al-Rawi1, Vanessa Hug1, Silvia Diabaté1, Stephan L Grage4, Matthias Meffert5, Tobias Stoeger6, Dagmar Gerthsen5, Anne S Ulrich4, Christof M Niemeyer3, Carsten Weiss1.
Abstract
Here, amorphous silica nanoparticles (NPs), one of the most abundant nanomaterials, are used as an example to illustrate the utmost importance of surface coverage by functional groups which critically determines biocompatibility. Silica NPs are functionalized with increasing amounts of amino groups, and the number of surface exposed groups is quantified and characterized by detailed NMR and fluorescamine binding studies. Subsequent biocompatibility studies in the absence of serum demonstrate that, irrespective of surface modification, both plain and amine-modified silica NPs trigger cell death in RAW 264.7 macrophages. The in vitro results can be confirmed in vivo and are predictive for the inflammatory potential in murine lungs. In the presence of serum proteins, on the other hand, a replacement of only 10% of surface-active silanol groups by amines is sufficient to suppress cytotoxicity, emphasizing the relevance of exposure conditions. Mechanistic investigations identify a key role of lysosomal injury for cytotoxicity only in the presence, but not in the absence, of serum proteins. In conclusion, this work shows the critical need to rigorously characterize the surface coverage of NPs by their constituent functional groups, as well as the impact of serum, to reliably establish quantitative nanostructure activity relationships and develop safe nanomaterials.Entities:
Keywords: cytotoxicity; macrophages; silica nanoparticles; surface-characterization; surface-functionalization
Year: 2019 PMID: 30721573 DOI: 10.1002/smll.201805400
Source DB: PubMed Journal: Small ISSN: 1613-6810 Impact factor: 13.281