| Literature DB >> 27441789 |
Ioannis G Theodorou1, Pakatip Ruenraroengsak1,2, Andrew Gow3, Stephan Schwander4, Junfeng Jim Zhang5, Kian Fan Chung2, Teresa D Tetley2, Mary P Ryan1, Alexandra E Porter1.
Abstract
Inhaled nanoparticles (NPs) have high-deposition rates in the alveolar region of the lung but the effects of pulmonary surfactant (PS) on nanoparticle bioreactivity are unclear. Here, the impact of PS on the stability and dissolution of ZnO nanowires (ZnONWs) was investigated, and linked with their bioreactivity in vitro with human alveolar epithelial type 1-like cells (TT1). Pre-incubation of ZnONWs with Curosurf® (a natural porcine PS) decreased their dissolution at acidic pH, through the formation of a phospholipid corona. Confocal live cell microscopy confirmed that Curosurf® lowered intracellular dissolution, thus delaying the onset of cell death compared to bare ZnONWs. Despite reducing dissolution, Curosurf® significantly increased the uptake of ZnONWs within TT1 cells, ultimately increasing their toxicity after 24 h. Although serum improved ZnONW dispersion in suspension similar to Curosurf®, it had no effect on ZnONW internalization and toxicity, indicating a unique role of PS in promoting particle uptake. In the absence of PS, ZnONW length had no effect on dissolution kinetics or degree of cellular toxicity, indicating a less important role of length in determining ZnONW bioreactivity. This work provides unique findings on the effects of PS on the stability and toxicity of ZnONWs, which could be important in the study of pulmonary toxicity and epithelial-endothelial translocation of nanoparticles in general.Entities:
Keywords: Alveoli; Curosurf®; epithelial uptake; nanoparticles; nanotoxicity
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Year: 2016 PMID: 27441789 PMCID: PMC5322737 DOI: 10.1080/17435390.2016.1214762
Source DB: PubMed Journal: Nanotoxicology ISSN: 1743-5390 Impact factor: 5.913