| Literature DB >> 32179334 |
Shisan Xu1, Huan Zhang2, Ping-Chieh Pao3, Audrey Lee3, Jun Wang3, Yu Suen Chan4, Francis A M Manno Iii5, Shun Wan Chan6, Shuk Han Cheng7, Xueping Chen8.
Abstract
Phthalates are commonly used in plastic products in daily life. The endocrine-disrupting effects of phthalates have been widely reported. Accumulating evidence from human cohorts and lab animals indicate exposure to phthalates might impair neurodevelopment. However, the direct causal relationship and mechanism between phthalates with neurodevelopment and neurotoxicity have not been firmly established. We found that phthalates (i.e. DBP, DINP, BBP) disrupted the expression of estrogen receptors (esr1, esr2a, esr2b), and impaired neurogenesis in the brain of zebrafish during embryonic development. Moreover, the abnormal expression of estrogen receptors, especially esr2a, was partly rescued in zebrafish which exposed to phthalates, with the estrogen receptor antagonist tamoxifen. Hence, impaired neurogenesis of zebrafish exposed to phthalates was partly reversed by tamoxifen treatment. Moreover, our results show that induced pluripotent stem cells (iPSC)-derived human neurons exposed to phthalates triggered double-strand DNA breaks in vitro. Overall, this study demonstrates that exposure to phthalates affects neurodevelopment in zebrafish embryos and induces neurotoxicity in human neurons partly through disrupting the expression of estrogen receptors.Entities:
Keywords: Double-Strand DNA break; Estrogen receptor; Estrogenic activity; Neurodevelopment; Neurons; Phthalates; Zebrafish
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Year: 2020 PMID: 32179334 DOI: 10.1016/j.aquatox.2020.105469
Source DB: PubMed Journal: Aquat Toxicol ISSN: 0166-445X Impact factor: 4.964