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Male autism spectrum disorder is linked to brain aromatase disruption by prenatal BPA in multimodal investigations and 10HDA ameliorates the related mouse phenotype.

journal contribution
posted on 2024-09-22, 23:52 authored by Christos Symeonides, Kristina Vacy, Sarah Thomson, Sam Tanner, Hui Kheng Chua, Shilpi Dixit, Toby MansellToby Mansell, Martin O'HelyMartin O'Hely, Boris NovakovicBoris Novakovic, Julie B Herbstman, Shuang Wang, Jia Guo, Jessalynn Chia, Nhi Thao Tran, Sang Eun Hwang, Kara Britt, Feng Chen, Tae Hwan Kim, Christopher A Reid, Anthony El-Bitar, Gabriel B Bernasochi, Lea M Durham Delbridge, Vincent R Harley, Yann W Yap, Deborah Dewey, Chloe J Love, David BurgnerDavid Burgner, Mimi TangMimi Tang, Peter SlyPeter Sly, Richard SafferyRichard Saffery, Jochen F Mueller, Nicole Rinehart, Bruce Tonge, Peter VuillerminPeter Vuillermin, BIS Investigator Group, Anne-Louise Ponsonby, Wah Chin Boon
Male sex, early life chemical exposure and the brain aromatase enzyme have been implicated in autism spectrum disorder (ASD). In the Barwon Infant Study birth cohort (n = 1074), higher prenatal maternal bisphenol A (BPA) levels are associated with higher ASD symptoms at age 2 and diagnosis at age 9 only in males with low aromatase genetic pathway activity scores. Higher prenatal BPA levels are predictive of higher cord blood methylation across the CYP19A1 brain promoter I.f region (P = 0.009) and aromatase gene methylation mediates (P = 0.01) the link between higher prenatal BPA and brain-derived neurotrophic factor methylation, with independent cohort replication. BPA suppressed aromatase expression in vitro and in vivo. Male mice exposed to mid-gestation BPA or with aromatase knockout have ASD-like behaviors with structural and functional brain changes. 10-hydroxy-2-decenoic acid (10HDA), an estrogenic fatty acid alleviated these features and reversed detrimental neurodevelopmental gene expression. Here we demonstrate that prenatal BPA exposure is associated with impaired brain aromatase function and ASD-related behaviors and brain abnormalities in males that may be reversible through postnatal 10HDA intervention.

Funding

Determinants and cardiometabolic consequences of early life inflammation : National Health and Medical Research Council | 1175744

History

Pagination

6367-

Volume

15

Publisher

Springer Nature

Issue

1

Journal

Nat Commun

Language

eng

Location

England

Medium

Electronic

Number

6367

PII

10.1038/s41467-024-48897-8

Publisher licence

CC BY

Online publication date

2024-08-07

Publication date

2024-08-07

Associated identifiers

grant.9854185 (dimensions-grant-id)

Publication status

  • Published online