Distinct genetic regions are associated with differential population susceptibility to chemical exposures

Distinct genetic regions are associated with differential population susceptibility to chemical exposures

Interactions between environmental factors and genetics underlie the majority of chronic human diseases. Chemical exposures are likely an underestimated contributor, yet gene-environment (GxE) interaction studies rarely assess their modifying effects. Here, we describe a novel method to profile the...

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Main Authors: Marissa B. Kosnik, Stefan Enroth, Oskar Karlsson
Format: Article
Language:English
Published: Elsevier 2021-07-01
Series:Environment International
Subjects:
Chemical exposures
Risk assessment
Gene-environment interactions
New approach methodologies
Consumer products
Data integration
Online Access:http://www.sciencedirect.com/science/article/pii/S0160412021001136
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spelling doaj-6b2c9c9c922741ac9a0d603261ff9fb12021-04-18T06:16:01ZengElsevierEnvironment International0160-41202021-07-01152106488Distinct genetic regions are associated with differential population susceptibility to chemical exposuresMarissa B. Kosnik0Stefan Enroth1Oskar Karlsson2Science for Life Laboratory, Department of Environmental Science, Stockholm University, 114 18 Stockholm, Sweden; Corresponding author.Department of Immunology, Genetics, and Pathology, Biomedical Center, Science for Life Laboratory Uppsala, Uppsala University, 751 85 Uppsala, SwedenScience for Life Laboratory, Department of Environmental Science, Stockholm University, 114 18 Stockholm, SwedenInteractions between environmental factors and genetics underlie the majority of chronic human diseases. Chemical exposures are likely an underestimated contributor, yet gene-environment (GxE) interaction studies rarely assess their modifying effects. Here, we describe a novel method to profile the human genome and identify regions associated with differential population susceptibility to chemical exposures. Single nucleotide polymorphisms (SNPs) implicated in enriched chemical-disease intersections were identified and validated for three chemical classes with expected GxE interaction potential (neuroactive, hepatoactive, and cardioactive compounds). The same approach was then used to characterize consumer product classes with unknown risk for GxE interactions (washing products, cosmetics, and adhesives). Additionally, high-risk variant sets that may confer differential population susceptibility were identified for these consumer product groups through frequent itemset mining and pathway analysis. A dataset of 2454 consumer product chemical-disease linkages, with risk values, SNPs, and pathways for each association was developed, describing the interplay between environmental factors and genetics in human disease progression. We found that genetic hotspots implicated in GxE interactions differ across chemical classes (e.g., washing products had high-risk SNPs implicated in nervous system disease) and illustrate how this approach can discover new associations (e.g., washing product n-butoxyethanol implicated SNPs in the PI3K-Akt signaling pathway for Alzheimer’s disease). Hence, our approach can predict high-risk genetic regions for differential population susceptibility to chemical exposures and characterize chemical modifying factors in specific diseases. These methods show promise for describing how chemical exposures can lead to varied health outcomes in a population and for incorporating inter-individual variability into chemical risk assessment.http://www.sciencedirect.com/science/article/pii/S0160412021001136Chemical exposuresRisk assessmentGene-environment interactionsNew approach methodologiesConsumer productsData integration
collection DOAJ
language English
format Article
sources DOAJ
author Marissa B. Kosnik
Stefan Enroth
Oskar Karlsson
spellingShingle Marissa B. Kosnik
Stefan Enroth
Oskar Karlsson
Distinct genetic regions are associated with differential population susceptibility to chemical exposures
Environment International
Chemical exposures
Risk assessment
Gene-environment interactions
New approach methodologies
Consumer products
Data integration
author_facet Marissa B. Kosnik
Stefan Enroth
Oskar Karlsson
author_sort Marissa B. Kosnik
title Distinct genetic regions are associated with differential population susceptibility to chemical exposures
title_short Distinct genetic regions are associated with differential population susceptibility to chemical exposures
title_full Distinct genetic regions are associated with differential population susceptibility to chemical exposures
title_fullStr Distinct genetic regions are associated with differential population susceptibility to chemical exposures
title_full_unstemmed Distinct genetic regions are associated with differential population susceptibility to chemical exposures
title_sort distinct genetic regions are associated with differential population susceptibility to chemical exposures
publisher Elsevier
series Environment International
issn 0160-4120
publishDate 2021-07-01
description Interactions between environmental factors and genetics underlie the majority of chronic human diseases. Chemical exposures are likely an underestimated contributor, yet gene-environment (GxE) interaction studies rarely assess their modifying effects. Here, we describe a novel method to profile the human genome and identify regions associated with differential population susceptibility to chemical exposures. Single nucleotide polymorphisms (SNPs) implicated in enriched chemical-disease intersections were identified and validated for three chemical classes with expected GxE interaction potential (neuroactive, hepatoactive, and cardioactive compounds). The same approach was then used to characterize consumer product classes with unknown risk for GxE interactions (washing products, cosmetics, and adhesives). Additionally, high-risk variant sets that may confer differential population susceptibility were identified for these consumer product groups through frequent itemset mining and pathway analysis. A dataset of 2454 consumer product chemical-disease linkages, with risk values, SNPs, and pathways for each association was developed, describing the interplay between environmental factors and genetics in human disease progression. We found that genetic hotspots implicated in GxE interactions differ across chemical classes (e.g., washing products had high-risk SNPs implicated in nervous system disease) and illustrate how this approach can discover new associations (e.g., washing product n-butoxyethanol implicated SNPs in the PI3K-Akt signaling pathway for Alzheimer’s disease). Hence, our approach can predict high-risk genetic regions for differential population susceptibility to chemical exposures and characterize chemical modifying factors in specific diseases. These methods show promise for describing how chemical exposures can lead to varied health outcomes in a population and for incorporating inter-individual variability into chemical risk assessment.
topic Chemical exposures
Risk assessment
Gene-environment interactions
New approach methodologies
Consumer products
Data integration
url http://www.sciencedirect.com/science/article/pii/S0160412021001136
work_keys_str_mv AT marissabkosnik distinctgeneticregionsareassociatedwithdifferentialpopulationsusceptibilitytochemicalexposures
AT stefanenroth distinctgeneticregionsareassociatedwithdifferentialpopulationsusceptibilitytochemicalexposures
AT oskarkarlsson distinctgeneticregionsareassociatedwithdifferentialpopulationsusceptibilitytochemicalexposures
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