Abstract
The increasing manufacture and use of products based on nanotechnology raises concerns for both workers and consumers. Various studies report induction of pulmonary inflammation after inhalation exposure to nanoparticles, which can vary in aspects such as size, shape, charge, crystallinity, chemical composition, and dissolution rate. Each of these aspects can affect their toxicity, although it is largely unknown to what extent. The aim of the current review is to analyse published data on inhalation of nanoparticles to identify and evaluate the contribution of their physicochemical characteristics to the onset and development of pulmonary inflammation. Many physicochemical characteristics of nanoparticles affect their lung deposition, clearance, and pulmonary response that, in combination, ultimately determine whether pulmonary inflammation will occur and to what extent. Lung deposition is mainly determined by the physical properties of the aerosol (size, density, shape, hygroscopicity) in relation to airflow and the anatomy of the respiratory system, whereas clearance and translocation of nanoparticles are mainly determined by their geometry and surface characteristics. Besides size and chemical composition, other physicochemical characteristics influence the induction of pulmonary inflammation after inhalation. As some nanoparticles dissolve, they can release toxic ions that can damage the lung tissue, making dissolution rate an important characteristic that affects lung inflammation. Fibre-shaped materials are more toxic to the lungs compared to spherical shaped nanoparticles of the same chemical composition. In general, cationic nanoparticles are more cytotoxic than neutral or anionic nanoparticles. Finally, surface reactivity correlates well with observed pulmonary inflammation. With all these characteristics affecting different stages of the events leading to pulmonary inflammation, no unifying dose metric could be identified to describe pulmonary inflammation for all nanomaterials, although surface reactivity might be a useful measure. To determine the extent to which the various characteristics influence the induction of pulmonary inflammation, the effect of these characteristics on lung deposition, clearance, and pulmonary response should be systematically evaluated. The results can then be used to facilitate risk assessment by categorizing nanoparticles according to their characteristics.
Highlights
In recent years, a large number of nanotechnologyenabled products have entered the global marketplace
Several in vivo inhalation studies report decreased clearance of nanoparticles from the lungs compared to larger-sized particles, resulting in increased retention time [32,69,70,73]
Another study observed that carbon black generated substantial amounts of reactive oxygen species (ROS) under cell-free conditions, but titanium dioxide nanoparticles did not. Both showed a comparable dose-dependent capacity to produce intracellular ROS [141]. These results suggest that the generation of ROS might be an indirect effect of the interaction of the nanoparticles with cellular components
Summary
A large number of nanotechnologyenabled products have entered the global marketplace. Several in vivo inhalation studies report decreased clearance of nanoparticles from the lungs compared to larger-sized particles, resulting in increased retention time [32,69,70,73]. When rats were exposed for 6 hours by inhalation to titanium dioxide particles with a primary size of 5 nm and an agglomerate size of 30 nm (small agglomerates) or 190 nm (large agglomerates), there was an effect of agglomerate size on pulmonary inflammation [18] Exposures to both small and large agglomerates at 7 mg/m3 resulted in a lung burden of 51.3 and 51.5 μg, respectively and induced increased lactate dehydrogenase (LDH) and oxidative stress markers.
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