TY  - JOUR
A1  - Graf, Philipp
A1  - Mantion, Alexandre
A1  - Haase, Andrea
A1  - Thuenemann, Andreas F.
A1  - Masic, Admir
A1  - Meier, Wolfgang P.
A1  - Luch, Andreas
A1  - Taubert, Andreas
T1  - Silicification of peptide-coated silver nanoparticles-A biomimetic soft chemistry approach toward chiral hybrid core-shell materials
JF  - ACS nano
N2  - Silica and silver nanoparticles are relevant materials for new applications in optics, medicine, and analytical chemistry. We have previously reported the synthesis of pH responsive, peptide-templated, chiral silver nanoparticles. The current report shows that peptide-stabilized nanoparticles can easily be coated with a silica shell by exploiting the ability of the peptide coating to hydrolyze silica precursors such as TEOS or TMOS. The resulting silica layer protects the nanoparticles from chemical etching, allows their inclusion in other materials, and renders them biocompatible. Using electron and atomic force microscopy, we show that the silica shell thickness and the particle aggregation can be controlled simply by the reaction time. Small-angle X ray scattering confirms the Ag/peptide@silica core-shell structure. UV-vis and circular dichroism spectroscopy prove the conservation of the silver nanoparticle chirality upon silicification. Biological tests show that the biocompatibility in simple bacterial systems is significantly improved once a silica layer is deposited on the silver particles.
KW  - peptide-templated materials
KW  - silver nanoparticles
KW  - chiral nanoparticles
KW  - Ag/peptide@SiO(2) nanostructures
KW  - core-shell structures
Y1  - 2011
U6  - https://doi.org/10.1021/nn102969p
SN  - 1936-0851
VL  - 5
IS  - 2
SP  - 820
EP  - 833
PB  - American Chemical Society
CY  - Washington
ER  - 
TY  - JOUR
A1  - Haase, Andrea
A1  - Rott, Stephanie
A1  - Mantion, Alexandre
A1  - Graf, Philipp
A1  - Plendl, Johanna
A1  - Thünemann, Andreas F.
A1  - Meier, Wolfgang P.
A1  - Taubert, Andreas
A1  - Luch, Andreas
A1  - Reiser, Georg
T1  - Effects of silver nanoparticles on primary mixed neural cell cultures: Uptake, oxidative stress and acute calcium responses
JF  - Toxicological sciences
N2  - In the body, nanoparticles can be systemically distributed and then may affect secondary target organs, such as the central nervous system (CNS). Putative adverse effects on the CNS are rarely investigated to date. Here, we used a mixed primary cell model consisting mainly of neurons and astrocytes and a minor proportion of oligodendrocytes to analyze the effects of well-characterized 20 and 40 nm silver nanoparticles (SNP). Similar gold nanoparticles served as control and proved inert for all endpoints tested. SNP induced a strong size-dependent cytotoxicity. Additionally, in the low concentration range (up to 10 mu g/ml of SNP), the further differentiated cultures were more sensitive to SNP treatment. For detailed studies, we used low/medium dose concentrations (up to 20 mu g/ml) and found strong oxidative stress responses. Reactive oxygen species (ROS) were detected along with the formation of protein carbonyls and the induction of heme oxygenase-1. We observed an acute calcium response, which clearly preceded oxidative stress responses. ROS formation was reduced by antioxidants, whereas the calcium response could not be alleviated by antioxidants. Finally, we looked into the responses of neurons and astrocytes separately. Astrocytes were much more vulnerable to SNP treatment compared with neurons. Consistently, SNP were mainly taken up by astrocytes and not by neurons. Immunofluorescence studies of mixed cell cultures indicated stronger effects on astrocyte morphology. Altogether, we can demonstrate strong effects of SNP associated with calcium dysregulation and ROS formation in primary neural cells, which were detectable already at moderate dosages.
KW  - silver nanoparticles
KW  - neurons
KW  - oxidative stress
KW  - protein carbonyls
KW  - calcium
Y1  - 2012
U6  - https://doi.org/10.1093/toxsci/kfs003
SN  - 1096-6080
VL  - 126
IS  - 2
SP  - 457
EP  - 468
PB  - Oxford Univ. Press
CY  - Oxford
ER  - 
TY  - JOUR
A1  - Lutze, Jana
A1  - Bañares, Miguel A.
A1  - Pita, Marcos
A1  - Haase, Andrea
A1  - Luch, Andreas
A1  - Taubert, Andreas
T1  - alpha-((4-Cyanobenzoyl)oxy)-omega-methyl poly(ethylene glycol)
BT  - a new stabilizer for silver nanoparticles
JF  - Beilstein journal of nanotechnology
N2  - The article describes the synthesis and properties of alpha-((4-cyanobenzoyl)oxy)-omega-methyl poly(ethylene glycol), the first poly(ethylene glycol) stabilizer for metal nanoparticles that is based on a cyano rather than a thiol or thiolate anchor group. The silver particles used to evaluate the effectiveness of the new stabilizer typically have a bimodal size distribution with hydrodynamic diameters of ca. 13 and ca. 79 nm. Polymer stability was evaluated as a function of the pH value both for the free stabilizer and for the polymers bound to the surface of the silver nanoparticles using H-1 NMR spectroscopy and zeta potential measurements. The polymer shows a high stability between pH 3 and 9. At pH 12 and higher the polymer coating is degraded over time suggesting that alpha-((4-cyanobenzoyl) oxy)-omega-methyl poly(ethylene glycol) is a good stabilizer for metal nanoparticles in aqueous media unless very high pH conditions are present in the system. The study thus demonstrates that cyano groups can be viable alternatives to the more conventional thiol/thiolate anchors.
KW  - cyano anchor group
KW  - poly(ethylene glycol)
KW  - polymer coating
KW  - silver nanoparticles
Y1  - 2017
U6  - https://doi.org/10.3762/bjnano.8.67
SN  - 2190-4286
VL  - 8
SP  - 627
EP  - 635
PB  - Beilstein-Institut zur Förderung der Chemischen Wissenschaften
CY  - Frankfurt, Main
ER  -