# Effects of combined prenatal exposure to air pollution and maternal stress on social behavior and oxytocin and vasopressin systems in male and female mice

**Authors:** Maura C. Stoehr, Elise M. Martin, Joy T. Babalola, Jason Xue, Matthew J. Kern, Niki Y. Li, Madeline F. Winters, Sarvin Bhagwagar, Caroline J. Smith

PMC · DOI: 10.1111/jne.70151 · Journal of Neuroendocrinology · 2026-03-05

## TL;DR

Exposure to air pollution and maternal stress during pregnancy affects social behavior in mice, with changes in brain receptors linked to social behavior.

## Contribution

This study reveals sex-specific effects of combined prenatal exposure on social behavior and V1aR expression in mice.

## Key findings

- DEP/MS exposure reduced social interaction time in male mice and social novelty preference in females.
- Avpr1a mRNA was significantly increased in the nucleus accumbens in both sexes after DEP/MS exposure.
- No changes in OXT or AVP cell number or fiber density were observed in hypothalamic regions.

## Abstract

Prenatal exposures to air pollution and maternal psychosocial stress are each associated with increased risk of neurodevelopmental disorders, including autism spectrum disorder (ASD), and epidemiological work suggests that concurrent exposure to these risk factors may be particularly harmful. This is important given that the same populations often bear the brunt of both toxicant and psychosocial stress burdens. Social impairments are a defining symptom in ASD. Previous work modeling combined prenatal exposure to diesel exhaust particles (DEPs) and maternal stress (MS) in rodents has found male‐biased social deficits in offspring, as well as changes to neuroimmune processes and the gut microbiome. However, the precise neural circuits on which these exposures converge to impact social behavior are unclear. Oxytocin (OXT) and vasopressin (AVP) are neuropeptides critical to the regulation of social behavior across species, signaling primarily at the oxytocin receptor (Oxtr) and vasopressin V1a receptor (V1aR) in the brain. Here, we hypothesized that OXT and/or AVP expression would be reduced in the brain following DEP/MS exposure. Following prenatal exposure to DEP/MS or the vehicle/control condition (VEH/CON), we measured maternal and offspring outcomes during the perinatal period, social and anxiety‐like behavior during adolescence, OXT and AVP cell/fiber density, and Oxtr and Avpr1a mRNA expression in early adulthood in several brain regions in both males and females. We observed a decrease in interaction time in DEP/MS males as compared to VEH/CON in the sociability assay and a decrease in social novelty preference in DEP/MS females as compared to VEH/CON. No effects of sex or treatment were observed on OXT or AVP cell number or fiber density in the hypothalamic regions assessed. However, numerous sex differences were observed in Oxtr and Avpr1a mRNA. Moreover, Avpr1a mRNA was significantly increased following DEP/MS exposure in the nucleus accumbens in both sexes and trended towards increasing in the dorsal hippocampus. Together, these findings suggest that DEP/MS exposure has a stronger impact on female social behavior than previously observed. Moreover, while DEP/MS exposure does not appear to impact OXT or AVP expression in the brain, V1aR expression is modulated by DEP/MS exposure in the nucleus accumbens.

## Linked entities

- **Genes:** OXTR (oxytocin receptor) [NCBI Gene 5021], AVPR1A (arginine vasopressin receptor 1A) [NCBI Gene 552]
- **Proteins:** OXT (oxytocin/neurophysin I prepropeptide), avp (arginine vasopressin)
- **Diseases:** autism spectrum disorder (MONDO:0005258)
- **Species:** Mus musculus (taxon 10090)

## Full-text entities

- **Genes:** Oxtr (oxytocin receptor) [NCBI Gene 25342] {aka OT-R, OTR, OTR1}, Oxt (oxytocin) [NCBI Gene 18429] {aka OT, Oxy}, Avp (arginine vasopressin) [NCBI Gene 11998] {aka Vp, Vsp}, Avpr1a (arginine vasopressin receptor 1A) [NCBI Gene 25107] {aka AVPR, V1a, V1aR}, Avpr1a (arginine vasopressin receptor 1A) [NCBI Gene 54140] {aka AVPR, Avpr1, V1a, V1aR}, Oxtr (oxytocin receptor) [NCBI Gene 18430] {aka OTR}
- **Diseases:** ASD (MESH:D000067877), neurodevelopmental and/or psychiatric disorders (MESH:D001523), disrupted neurodevelopment (MESH:D019958), autism (MESH:D001321), anxiety (MESH:D001007), asthma (MESH:D001249), weight gain (MESH:D015430), social deficits (MESH:D009461), MS (MESH:D000079225), neurodevelopmental insults (MESH:D008607), Social impairments (OMIM:300082), aggression (MESH:D010554), DEP (MESH:D006359), neurodevelopmental disorders (MESH:D002658), MIA (MESH:D000079262)
- **Chemicals:** Aroclor 1221 (MESH:C032739), E2 (MESH:D004958), N (MESH:D009584), Triton-X (MESH:D017830), phenol (MESH:D019800), H2O (MESH:D014867), isoflurane (MESH:D007530), bisphenol A (MESH:C006780), Trizol (MESH:C411644), isopropanol (MESH:D019840), ethanol (MESH:D000431), polycyclic aromatic hydrocarbon (MESH:D011084), aluminum (MESH:D000535), H2O2 (MESH:D006861), DEP (-), sodium citrate (MESH:D000077559), polychlorinated biphenyl (MESH:D011078), plastics (MESH:D010969), chlorpyrifos (MESH:D004390), 2-methylbutane (MESH:C067038), CO2 (MESH:D002245), sucrose (MESH:D013395), paraformaldehyde (MESH:C003043), LPS (MESH:D008070), chloroform (MESH:D002725), Tween20 (MESH:D011136), sodium tetraborate (MESH:C010634), PBS (MESH:D007854), 4', 6-Diamidino-2-phenylindole (MESH:C007293)
- **Species:** Mus musculus (house mouse, species) [taxon 10090], Rattus norvegicus (brown rat, species) [taxon 10116], Bacteroides (genus) [taxon 816], Homo sapiens (human, species) [taxon 9606], Microtus ochrogaster (prairie vole, species) [taxon 79684], Cavia porcellus (domestic guinea pig, species) [taxon 10141], Limosilactobacillus reuteri (species) [taxon 1598], gut metagenome (species) [taxon 749906]

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## References

118 references — full list in the complete paper: https://tomesphere.com/paper/PMC12963532/full.md

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Source: https://tomesphere.com/paper/PMC12963532