Reconstructing population exposures to acrylamide from human monitoring data using a pharmacokinetic framework

Yu-Sheng Lin; Viktor Morozov; Abdel-Razak Kadry; James L Caffrey; Wei-Chun Chou

doi:10.1016/j.chemosphere.2023.138798

Reconstructing population exposures to acrylamide from human monitoring data using a pharmacokinetic framework

Chemosphere. 2023 Aug:331:138798. doi: 10.1016/j.chemosphere.2023.138798. Epub 2023 May 1.

Authors

Yu-Sheng Lin¹, Viktor Morozov², Abdel-Razak Kadry³, James L Caffrey⁴, Wei-Chun Chou⁵

Affiliations

¹ Office of Research and Development, US Environmental Protection Agency, Washington, DC, 20460, USA. Electronic address: Lin.Yu-Sheng@epa.gov.
² Office of Research and Development, US Environmental Protection Agency, Washington, DC, 20460, USA.
³ School of Public Health, University of Maryland, College Park, MD, 20742, USA.
⁴ Institute of Cardiovascular and Metabolic Diseases, University of North Texas Health Science Center, Fort Worth, TX, 76107, USA.
⁵ College of Public Health and Health Professions, University of Florida, Gainesville, FL, 32611, USA.

PMID: 37137393
DOI: 10.1016/j.chemosphere.2023.138798

Abstract

Background: Acrylamide toxicity involves several metabolic pathways. Thus, a panel of blood and urinary biomarkers for the evaluation of acrylamide exposure was deemed appropriate.

Objective: The study was designed to evaluate daily acrylamide exposure in US adults via hemoglobin adducts and urinary metabolites using a pharmacokinetic framework.

Methods: A cohort of 2798 subjects aged 20-79 was selected from the National Health and Nutrition Examination Survey (NHANES, 2013-2016) for analysis. Three acrylamide biomarkers including hemoglobin adducts of acrylamide in blood and two urine metabolites, N-Acetyl-S-(2-carbamoylethyl)cysteine (AAMA) and N-Acetyl-S-(2-carbamoyl-2-hydroxyethyl)-l-cysteine (GAMA) were used to estimate daily acrylamide exposure using validated pharmacokinetic prediction models. Multivariate regression models were also used to examine key factors in determining estimated acrylamide intake.

Results: The estimated daily acrylamide exposure varied across the sampled population. Estimated acrylamide daily exposure was comparable among the three different biomarkers (median: 0.4-0.7 μg/kg/d). Cigarette smoking emerged as the leading contributor to the acquired acrylamide dose. Smokers had the highest estimated acrylamide intake (1.20-1.49 μg/kg/d) followed by passive smokers (0.47-0.61) and non-smokers (0.45-0.59). Several covariates, particularly, body mass index and race/ethnicity, played roles in determining estimated exposures.

Discussion: Estimated daily acrylamide exposures among US adults using multiple acrylamide biomarkers were similar to populations reported elsewhere providing additional support for using the current approach in assessing acrylamide exposure. This analysis assumes that the biomarkers used indicate intake of acrylamide into the body, which is consistent with the substantial known exposures due to diet and smoking. Although this study did not explicitly evaluate background exposure arising from analytical or internal biochemical factors, these findings suggest that the use of multiple biomarkers may reduce uncertainties regarding the ability of any single biomarker to accurately represent actual systemic exposures to the agent. This study also highlights the value of integrating a pharmacokinetic approach into exposure assessments.

Keywords: Acrylamide; Biomarkers; Dose reconstruction; Hemoglobin adducts; Metabolites; Urine.

Published by Elsevier Ltd.

MeSH terms

Acetylcysteine*
Acrylamide* / toxicity
Adult
Biomarkers / urine
Hemoglobins
Humans
Nutrition Surveys

Substances

Acetylcysteine
Acrylamide
Biomarkers
Hemoglobins