Surface PEGylation suppresses pulmonary effects of CuO in allergen-induced lung inflammation.

BACKGROUND: Copper oxide (CuO) nanomaterials are used in a wide range of industrial and commercial applications. These materials can be hazardous, especially if they are inhaled. As a result, the pulmonary effects of CuO nanomaterials have been studied in healthy subjects but limited knowledge exists today about their effects on lungs with allergic airway inflammation (AAI). The objective of this study was to investigate how pristine CuO modulates allergic lung inflammation and whether surface modifications can influence its reactivity. CuO and its carboxylated (CuO COOH), methylaminated (CuO NH3) and PEGylated (CuO PEG) derivatives were administered here on four consecutive days via oropharyngeal aspiration in a mouse model of AAI. Standard genome-wide gene expression profiling as well as conventional histopathological and immunological methods were used to investigate the modulatory effects of the nanomaterials on both healthy and compromised immune system. RESULTS: Our data demonstrates that although CuO materials did not considerably influence hallmarks of allergic airway inflammation, the materials exacerbated the existing lung inflammation by eliciting dramatic pulmonary neutrophilia. Transcriptomic analysis showed that CuO, CuO COOH and CuO NH3 commonly enriched neutrophil-related biological processes, especially in healthy mice. In sharp contrast, CuO PEG had a significantly lower potential in triggering changes in lungs of healthy and allergic mice revealing that surface PEGylation suppresses the effects triggered by the pristine material. CONCLUSIONS: CuO as well as its functionalized forms worsen allergic airway inflammation by causing neutrophilia in the lungs, however, our results also show that surface PEGylation can be a promising approach for inhibiting the effects of pristine CuO. Our study provides information for health and safety assessment of modified CuO materials, and it can be useful in the development of nanomedical applications.

Nanodiamonds of Different Surface Chemistry Influence the Toxicity and Differentiation of Rat Bone Mesenchymal Stem Cells In Vitro.

The nanodiamonds (NDs) have attracted much attention in biomedical applications due to their excellent magnetic and optical properties. However, comprehensive study of different surfacemodified NDs on toxicity and differentiation of mesenchymal stem cells are very deficient. In this study, three types of NDs, i.e., ND-COOH, ND-NH+3 and ND-PEG were co-cultured with rat bone mesenchymal stem cells (MSCs) to assess their biosafety and effects on differentiation. In a dry state, they had a similar diameter of about 6-7 nm, and aggregated into ˜100 nm (hydrodynamic size) in cell culture medium. Co-culture with MSCs showed that the ND-COOH and ND-PEG had lower cytotoxicity than ND-NH+3. Alkaline comet assay showed slight genotoxicity for all the NDs regardless of their surface coatings. The reactive oxygen species (ROS) test showed that the cytotoxicity and genotoxicity of NDs may be attributed to the NDs-mediated intracellular oxidative stress. All the NDs did not show significant impact on the osteogenic differentiation of MSCs, whereas the ND-COOH and ND-PEG slightly impaired the adipogenic differentiation. Taken together, these findings provide some momentous implications for the design of surface chemical structures of NDs for their applications in biological field.

Cytotoxic and Proinflammatory Effects of Metal-Based Nanoparticles on THP-1 Monocytes Characterized by Combined Proteomics Approaches.

Thorough characterization of toxic effects of nanoparticles (NP) is desirable due to the increasing risk of potential environmental contamination by NP. In the current study, we combined three recently developed proteomics approaches to assess the effects of Au, CuO, and CdTe NP on the innate immune system. The human monocyte cell line THP-1 was employed as a model. The anticancer drugs camptothecin and doxorubicin were used as positive controls for cell death, and lipopolysaccharide was chosen as a positive control for proinflammatory activation. Despite equivalent overall toxicity effect (50 ± 10% dead cells), the three NP induced distinctly different proteomics signatures, with the strongest effect being induced by CdTe NP, followed by CuO and gold NP. The CdTe toxicity mechanism involves down-regulation of topoisomerases. The effect of CuO NP is most reminiscent of oxidative stress and involves up-regulation of proteins involved in heat response. The gold NP induced up-regulation of the inflammatory mediator, NF-κB, and its inhibitor TIPE2 was identified as a direct target of gold NP. Furthermore, gold NP triggered activation of NF-κB as evidenced by phosphorylation of the p65 subunit. Overall, the combined proteomics approach described here can be used to characterize the effects of NP on immune cells.

The effects of folate-conjugated gold nanorods in combination with plasmonic photothermal therapy on mouth epidermal carcinoma cells.

The use of lasers has emerged to be highly promising for cancer therapy modalities, most commonly, the photothermal therapy method. Unfortunately, the most common disadvantage of laser therapy is its nonselectivity and requirement of high power density. The use of plasmonic nanoparticles as highly enhanced photoabsorbing agents has thus introduced a much more selective and efficient cancer therapy strategy. In this study, we aimed to demonstrate the selective targeting and destruction of mouth epidermal carcinoma cells (KB cells) using the photothermal therapy of folate-conjugated gold nanorods (F-GNRs). Considering the beneficial characteristics of GNRs and overexpression of the folate receptor by KB cells, we selected F-GNRs as a targeted photothermal therapy agent. Cell viability was evaluated using a 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assay. Apoptosis was determined by flow cytometry using an annexin V-fluorescein isothiocyanate/propidium iodide apoptosis detection kit. No cell damage or cytotoxicity from the individual treatment of laser light or F-GNRs was observed. However, a 56% cell lethality was achieved for KB cells using combined plasmonic photothermal therapy of 20 µM F-GNRs with seven pulses of laser light and 6-h incubation periods. Cell lethality strongly depends on the concentration of F-GNRs and the incubation period that is mainly due to the induction of apoptosis. This targeted damage is due to the F-GNRs present in the cancer cells strongly absorbing near-infrared laser light and rapidly converting it to heat. This new therapeutic avenue for cancer therapy merits further investigation using in vivo models for application in humans.

Exciton-plasmon interaction in a composite metal-insulator-semiconductor nanowire system.

We report about the synthesis and optical properties of a composite metal-insulator-semiconductor nanowire system which consists of a wet-chemically grown silver wire core surrounded by a SiO2 shell of controlled thickness, followed by an outer shell of highly luminescent CdSe nanocrystals. With microphotoluminescence (micro-PL) experiments, we studied the exciton-plasmon interaction in individual nanowires and analyzed the spatially resolved nanocrystal emission for different nanowire length, SiO2-shell thickness, nanocrystal shape, pump power, and emission polarization. For an SiO2 spacer thickness of approximately 15 nm, we observed an efficient excitation of surface plasmons by excitonic emission of CdSe nanocrystals. For nanowire lengths up to approximately 10 microm, the composite metal-insulator-semiconductor nanowires ((Ag)SiO2)CdSe act as a waveguide for 1D-surface plasmons at optical frequencies with efficient photon outcoupling at the nanowire tips, which is promising for efficient exciton-plasmon-photon conversion and surface plasmon guiding on a submicron scale in the visible spectral range.

Influence of titanium dioxide nanorods with different surface chemistry on the differentiation of rat bone marrow mesenchymal stem cells.

In this study, four kinds of TiO2 nanorods (TiO2 NRs), with similar aspect ratios but different surface functional groups, i.e. amines (-NH2), carboxyl groups (-COOH) and poly(ethylene glycol) (-PEG), were used to study their interaction with rat bone marrow stem cells (MSCs). The aspect ratios of the TiO2 NRs were measured (50 to 65 nm in length and 8 nm in width) under transmission electron microscopy (TEM). The cellular uptake of the TiO2 NRs was qualitatively studied by TEM and then quantified by inductively coupled plasma mass spectrometry (ICP-MS). The results showed that the MSCs ingested larger amounts of TiO2-core NRs and TiO2-NH2 NRs than those of TiO2-COOH NRs and TiO2-PEG NRs, with similar intracellular distribution patterns. TiO2-core NRs induced the highest cytotoxicity, as a result of the highest intracellular level of reactive oxygen species (ROS), which was lowered upon surface functionalization. The genotoxicity of the TiO2 NRs was neglectable at tested concentrations, studied by the comet assay. The adipogenic and osteogenic differentiation potentials of the MSCs were firstly evaluated in terms of lipid droplet formation and calcium deposition respectively in the presence of the TiO2 NRs. All of the TiO2 NRs did not show an obvious influence on the adipogenic differentiation potential of the MSCs. But TiO2-COOH NRs showed a significant impairment on the osteogenic differentiation behaviors. The influence of TiO2 NRs on the osteogenic differentiation of the MSCs was further quantitatively studied by the expression of osteogenic markers (collagen type I and osteocalcein), at both gene and protein levels. The results confirmed the strongest hindrance of the osteogenic differentiation of the MSCs by TiO2-COOH NRs, due to the up-regulation of transforming growth factor beta 1 (TGF-ß1) and fibroblast growth factor (FGF-2). The results provide new information that the differentiation potential of the MSCs can be influenced by the presence of TiO2 NRs with different surface functionalities, suggesting a careful analysis of the biological impact of nanomaterials.

Surface plasmon mediated interference phenomena in low-q silver nanowire cavities.

Optical excitation of surface plasmons in wet-chemically grown monocrystalline silver nanowires ( approximately 100 nm diameter and up to a few tens of micrometers length) is studied by broadband imaging spectroscopy. Surface plasmons excited by an incident light beam in the so-called Kretschmann-Raether configuration give optical interference phenomena in the spectral domain. These spectral oscillations are interpreted in terms of Fabry-Perot cavity modes for surface plasmons in silver nanowires and allow for a direct experimental determination of the surface plasmon group velocity and cavity losses.

Colloidal quantum dots in all-dielectric high-Q pillar microcavities.

We have fabricated all-dielectric high-Q optical pillar resonators with embedded colloidal CdSe/ZnS quantum dots or rods as light emitters by focused ion beam milling. Three-dimensional light confinement and distinct pillar microcavity modes are observed. Results from a waveguide model for the mode patterns and their spectral positions are in excellent agreement with the experimental data. Cavities with elliptical cross sections show higher quality factors in the short axis direction than do circular resonators of the same cross-sectional area.