Literature DB >> 34890772

The behavioral effects of gestational and lactational benzo[a]pyrene exposure vary by sex and genotype in mice with differences at the Ahr and Cyp1a2 loci.

Amanda Honaker1, Angela Kyntchev1, Emma Foster1, Katelyn Clough1, Greg Hawk2, Emmanuella Asiedu1, Kevin Berling1, Emma DeBurger1, Mackenzie Feltner1, Victoria Ferguson1, Philip Tyler Forrest1, Kayla Jenkins1, Lisa Massie1, Jayasree Mullaguru1, Mame Diarra Niang1, Connor Perry1, Yvonne Sene1, Aria Towell1, Christine Perdan Curran3.   

Abstract

Benzo[a]pyrene (BaP) is a polycyclic aromatic hydrocarbon (PAH) and known carcinogen in the Top 10 on the United States' list of priority pollutants. Humans are exposed through a variety of sources including tobacco smoke, grilled foods and fossil fuel combustion. Recent studies of children exposed to higher levels of PAHs during pregnancy and early life have identified numerous adverse effects on the brain and behavior that persist into school age and adolescence. Our studies were designed to look for genotype and sex differences in susceptibility to gestational and lactational exposure to BaP using a mouse model with allelic differences in the aryl hydrocarbon receptor and the xenobiotic metabolizing enzyme CYP1A2. Pregnant dams were exposed to 10 mg/kg/day of BaP in corn oil-soaked cereal or the corn oil vehicle alone from gestational day 10 until weaning at postnatal day 25. Neurobehavioral testing began at P60 using one male and one female per litter. We found main effects of sex, genotype and treatment as well as significant gene x treatment and sex x treatment interactions. BaP-treated female mice had shorter latencies to fall in the Rotarod test. BaP-treated high-affinity AhrbCyp1a2(-/-) mice had greater impairments in Morris water maze. Interestingly, poor-affinity AhrdCyp1a2(-/-) mice also had deficits in spatial learning and memory regardless of treatment. We believe our findings provide future directions in identifying human populations at highest risk of early life BaP exposure, because our model mimics known human variation in our genes of interest. Our studies also highlight the value of testing both males and females in all neurobehavioral studies.
Copyright © 2021 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  Benzo[a]pyrene; Developmental neurotoxicity; Learning and memory; Motor deficits; PAH

Mesh:

Substances:

Year:  2021        PMID: 34890772      PMCID: PMC8763354          DOI: 10.1016/j.ntt.2021.107056

Source DB:  PubMed          Journal:  Neurotoxicol Teratol        ISSN: 0892-0362            Impact factor:   3.763


  54 in total

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