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Correlation of Regional Deposition Dosage for Inhaled Nanoparticles in Human and Rat Olfactory

journal contribution
posted on 2024-11-02, 02:43 authored by Lin TianLin Tian, Yidan Shang, Rui Chen, Ru Bai, Chunying Chen, Kiao InthavongKiao Inthavong, Jiyuan TuJiyuan Tu
Background Nose-to-brain transport of airborne ultrafine particles (UFPs) via the olfactory pathway has been verified as a possible route for particle translocation into the brain. The exact relationship between increased airborne toxicant exposure and neurological deterioration in the human central nervous system, is still unclear. However, the nasal olfactory is undoubtedly a critical junction where the time course and toxicant dose dependency might be inferred.MethodComputational fluid-particle dynamics modeling of inhaled nanoparticles (1 to 100nm) under low to moderate breathing conditions (5 to 14L/min - human; and 0.14 to 0.40L/min - rat) were performed in physiologically realistic human and rat nasal airways. The simulation emphasized olfactory deposition, and variations in airflow and particle flux caused by the inter-species airway geometry differences. Empirical equations were developed to predict regional deposition rates of inhaled nanoparticles on human and rat olfactory mucosa in sedentary breathing. Considering, breathing and geometric differences, quantified correlations between human and the rat olfactory deposition dose against a variety of metrics were proposed.ResultsRegional deposition of nanoparticles in human and the rat olfactory was extremely low, with the highest deposition (<3.5 and 8.1%) occurring for high diffusivity particles of 1.5nm and 5nm, respectively. Due to significant filtering of extremely small particles (<2nm) by abrupt sharp turns at front of the rat nose, only small fractions of the inhaled nanoparticles (in this range) reached rat olfactory than that in human (1.25 to 45%); however, for larger sizes (>3nm), significantly higher percentage of the inhaled nanoparticles reached rat nasal olfactory than that in human (2 to 32 folds). Taking into account the physical and geometric features between human and rat, the total deposition rate (#/min) and deposition rate per unit surface area (#/min/mm(2)) were comparable for particles>3nm. However, when body mass was considered, the normalized deposition rate (#/min/kg) in the rat olfactory region exceeded that in the human. Nanoparticles <1.5nm were filtered out by rat anterior nasal cavity, and therefore deposition in human olfactory region exceeded that in the rat model.ConclusionRegional deposition dose of inhaled nanoparticles in a human and rat olfactory region was governed by particle size and the breathing rate. Interspecies correlation was determined by combining the effect of deposition dosage, physical\geometric features, and genetic differences. Developed empirical equations provided a tool to quantify inhaled nanoparticle dose in human and rat nasal olfactory regions, which lay the ground work for comprehensive interspecies correlation between the two species. Furthermore, this study contributes to the fields in toxicology, i.e., neurotoxicity evaluation and risk assessment of UFPs, in long-term and low-dose inhalation exposure scenarios.

Funding

A multi-scale risk assessment platform for inhaled carbon nanotubes

Australian Research Council

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A Multiscale Modelling Platform for Nanoparticle Inhalation Risk Assessment

Australian Research Council

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History

Related Materials

  1. 1.
    DOI - Is published in 10.1186/s12989-019-0290-8
  2. 2.
    ISSN - Is published in 17438977

Journal

Particle and Fibre Toxicology

Volume

16

Number

6

Issue

6

Start page

1

End page

17

Total pages

17

Publisher

BioMed Central

Place published

United Kingdom

Language

English

Copyright

© The Author(s). 2019 Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License

Former Identifier

2006093669

Esploro creation date

2020-06-22

Fedora creation date

2019-10-23