3D Printer Particle Emissions: Translation to Internal Dose in Adults and Children

Peter Byrley; William K Boyes; Kim Rogers; Annie M Jarabek

doi:10.1016/j.jaerosci.2021.105765

3D Printer Particle Emissions: Translation to Internal Dose in Adults and Children

J Aerosol Sci. 2021 May 1:154:1-12. doi: 10.1016/j.jaerosci.2021.105765.

Authors

Peter Byrley¹, William K Boyes², Kim Rogers³, Annie M Jarabek¹

Affiliations

¹ Health and Environmental Effects Assessment Division (HEEAD), Center for Public Health and Environmental Assessment, Office of Research and Development (ORD), USEPA, RTP, NC 27711.
² Public Health and Integrated Toxicology Division (PHID), Center for Public Health and Environmental Assessment (CPHEA), Office of Research and Development (ORD), USEPA, RTP, NC 27711.
³ Watershed and Ecosystem Characterization Division (WECD), Center for Environmental Measurement and Modeling (CEMM), Office of Research and Development (ORD), USEPA, RTP, NC 27711.

Abstract

Desktop fused deposition modeling (FDM®) three-dimensional (3D) printers are becoming increasingly popular in schools, libraries, and among home hobbyists. FDM® 3D printers have been shown to release ultrafine airborne particles in large amounts, indicating the potential for inhalation exposure and consequent health risks among FDM® 3D printer users and other room occupants including children. These particles are generated from the heating of thermoplastic polymer feedstocks during the FDM® 3D printing process, with the most commonly used polymers being acrylonitrile butadiene styrene (ABS) and poly-lactic acid (PLA). Risk assessment of these exposures demands estimation of internal dose, especially to address intra-human variability across life stages. Dosimetry models have proven to effectively translate particle exposures to internal dose metrics relevant to evaluation of their effects in the respiratory tract. We used the open-access multiple path particle dosimetry (MPPD v3.04) model to estimate inhaled particle deposition in different regions of the respiratory tract for children of various age groups from three months to eighteen years old adults. Mass concentration data for input into the MPPD model were calculated using particle size distribution and density data from experimental FDM® 3D printer emissions tests using both ABS and PLA. The impact of changes in critical parameters that are principal determinants of inhaled dose, including: sex, age, and exposure duration, was examined using input parameter values available from the International Commission on Radiological Protection. Internal dose metrics used included regional mass deposition, mass deposition normalized by pulmonary surface area, surface area of deposited particles by pulmonary surface area, and retained regional mass. Total mass deposition was found to be highest in the 9-year-old to 18-year-old age groups with mass deposition by pulmonary surface area highest in 3-month-olds to 9-year-olds and surface area of deposited particles by pulmonary surface area to be highest in 9-year-olds. Clearance modeling revealed that frequent 3D printer users are at risk for an increased cumulative retained dose.

Keywords: 3D Printing; Dosimetry; Emissions; Inhalation; Respiratory; Translation.

Grants and funding

EPA999999/ImEPA/Intramural EPA/United States