Literature DB >> 24983898

Amphiphilic polymer-coated CdSe/ZnS quantum dots induce pro-inflammatory cytokine expression in mouse lung epithelial cells and macrophages.

Vivian Lee1, Ryan S McMahan, Xiaoge Hu, Xiaohu Gao, Elaine M Faustman, William C Griffith, Terrance J Kavanagh, David L Eaton, John K McGuire, William C Parks.   

Abstract

Quantum dots (Qdots) are semiconductor nanoparticles with size-tunable fluorescence capabilities with diverse applications. Qdots typically contain cadmium or other heavy metals, hence raising concerns of their potential toxicity, especially in occupational settings where inhalation of nanomaterials may increase the risk of lung disease. Accordingly, we assessed the effects of tri-n-octylphosphine oxide, poly(maleic anhydride-alt-1-tetradecene) (TOPO-PMAT) coated CdSe/ZnS Qdots on mouse lung epithelial cells and macrophages. Mouse tracheal epithelial cells (MTEC), grown as organotypic cultures, bone marrow-derived macrophages (BMDM), and primary alveolar macrophages (AM) were derived from C57BL/6J or A/J mice and treated with TOPO-PMAT CdSe/ZnS Qdots (10-160 nM) for up to 24 h. Cadmium analysis showed that Qdots remained in the apical compartment of MTEC cultures, whereas they were avidly internalized by AM and BMDM, which did not differ between strains. In MTEC, Qdots selectively induced expression (mRNA and protein) of neutrophil chemokines CXCL1 and CXCL2 but only low to no detectable levels of other factors assessed. In contrast, 4 h exposure to Qdots markedly increased expression of CXCL1, IL6, IL12, and other pro-inflammatory factors in BMDM. Higher inflammatory response was seen in C57BL/6J than in A/J BMDM. Similar expression responses were observed in AM, although overall levels were less robust than in BMDM. MTEC from A/J mice were more sensitive to Qdot pro-inflammatory effects while macrophages from C57BL/6J mice were more sensitive. These findings suggest that patterns of Qdot-induced pulmonary inflammation are likely to be cell-type specific and genetic background dependent.

Entities:  

Keywords:  Engineered nanomaterial; in vitro toxicity; pulmonary inflammation

Mesh:

Substances:

Year:  2014        PMID: 24983898      PMCID: PMC4669048          DOI: 10.3109/17435390.2014.930532

Source DB:  PubMed          Journal:  Nanotoxicology        ISSN: 1743-5390            Impact factor:   5.913


  27 in total

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Authors:  David K Scoville; Collin C White; Dianne Botta; Lisa A McConnachie; Megan E Zadworny; Stefanie C Schmuck; Xiaoge Hu; Xiaohu Gao; Jianbo Yu; Russell L Dills; Lianne Sheppard; Martha A Delaney; William C Griffith; Richard P Beyer; Richard C Zangar; Joel G Pounds; Elaine M Faustman; Terrance J Kavanagh
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Review 2.  In vitro to in vivo benchmark dose comparisons to inform risk assessment of quantum dot nanomaterials.

Authors:  Brittany A Weldon; William C Griffith; Tomomi Workman; David K Scoville; Terrance J Kavanagh; Elaine M Faustman
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Review 3.  Fluorescent Nanoparticles for Super-Resolution Imaging.

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4.  Epigenetic effects of cadmium in cancer: focus on melanoma.

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5.  The pulmonary inflammatory response to multiwalled carbon nanotubes is influenced by gender and glutathione synthesis.

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Review 7.  Applications and Immunological Effects of Quantum Dots on Respiratory System.

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8.  In vivo biodistribution and toxicology studies of cadmium-free indium-based quantum dot nanoparticles in a rat model.

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  8 in total

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