Increasing confidence in new approach methodologies for inhalation risk assessment with multiple end point assays using 5-day repeated exposure to 1,3-dichloropropene

Iru Paudel; A Rasim Barutcu; Raymond Samuel; Marjory Moreau; Scott D Slattery; Jamie Scaglione; Leslie Recio

doi:10.1016/j.tox.2023.153642

Increasing confidence in new approach methodologies for inhalation risk assessment with multiple end point assays using 5-day repeated exposure to 1,3-dichloropropene

Toxicology. 2023 Nov:499:153642. doi: 10.1016/j.tox.2023.153642. Epub 2023 Oct 18.

Authors

Iru Paudel¹, A Rasim Barutcu¹, Raymond Samuel¹, Marjory Moreau¹, Scott D Slattery¹, Jamie Scaglione¹, Leslie Recio²

Affiliations

¹ ScitoVation, LLC, 6 Davis Drive, Suite 146, Durham, NC 27709, USA.
² ScitoVation, LLC, 6 Davis Drive, Suite 146, Durham, NC 27709, USA. Electronic address: lRecio@scitovation.com.

PMID: 37863466
DOI: 10.1016/j.tox.2023.153642

Abstract

New Approach Methodologies (NAMs) are being widely used to reduce, refine, and replace, animal use in studying toxicology. For respiratory toxicology, this includes both in silico and in vitro alternatives to replace traditional in vivo inhalation studies. 1,3-Dichloropropene (1,3-DCP) is a volatile organic compound that is widely used in agriculture as a pre-planting fumigant. Short-term exposure of humans to 1,3-DCP can result in mucous membrane irritation, chest pain, headache, and dizziness. In our previous work, we exposed differentiated cells representing different parts of the respiratory epithelium to 1,3-DCP vapor, measured cytotoxicity, and did In Vitro to In Vivo Extrapolation (IVIVE). We have extended our previous study with 1,3-DCP vapors by conducting transcriptomics on acutely exposed nasal cultures and have implemented a separate 5-day repeated exposure with multiple endpoints to gain further molecular insight into our model. MucilAir™ Nasal cell culture models, representing the nasal epithelium, were exposed to six sub-cytotoxic concentrations of 1,3-DCP vapor at the air-liquid interface, and the nasal cultures were analyzed by different methodologies, including histology, transcriptomics, and glutathione (GSH) -depletion assays. We observed the dose-dependent effect of 1,3-DCP in terms of differential gene expression, change in cellular morphology from pseudostratified columnar epithelium to squamous epithelium, and depletion of GSH in MucilAir™ nasal cultures. The MucilAir™ nasal cultures were also exposed to 3 concentrations of 1,3-DCP using repeated exposure 4 h per day for 5 days and the histological analyses indicated changes in cellular morphology and a decrease in ciliated bodies and an increase in apoptotic bodies, with increasing concentrations of 1,3-DCP. Altogether, our results suggest that sub-cytotoxic exposures to 1,3-DCP lead to several molecular and cellular perturbations, providing significant insight into the mode-of-action (MoA) of 1,3-DCP using an innovative NAM model.

Keywords: 1; 3-Dichloropropene; Glutathione; IVIVE; Inhalation Toxicity; New Approach Methodology; PBPK modeling; Repeated Exposure MucilAir.

MeSH terms

Administration, Inhalation
Allyl Compounds* / metabolism
Allyl Compounds* / toxicity
Animals
Endpoint Determination
Humans
Hydrocarbons, Chlorinated* / toxicity
Inhalation Exposure / adverse effects
Pesticides*

Substances

1,3-dichloro-1-propene
Allyl Compounds
Hydrocarbons, Chlorinated
Pesticides