AI Article Synopsis
- The study investigates the effects of aryl-organophosphate flame retardants (OPFRs), TPhP and TDCIPP, on estrogen receptors, challenging the notion that traditional ERα binding assays fully explain their biological impacts.
- TPhP was identified as an ERα agonist that activates steroid receptor co-activators, whereas TDCIPP functions as an ERα antagonist; both compounds can activate the estrogen pathway via GPER in cells lacking ERα.
- The research demonstrates that both TPhP and TDCIPP enhance the synthesis of 17β-estradiol (E2) through different mechanisms, affecting the levels of other hormones and gene expression, thereby proposing frameworks for understanding their estrogen-disrupt
Article Abstract
As the typical aryl-organophosphate flame retardants (OPFRs), triphenyl phosphate (TPhP) and tris(1,3-dichloro-2-propyl) phosphate (TDCIPP) were reported to be estrogen disruptors. However, estrogen receptor α (ERα) binding experiments could not explain their biological effects. In this study, their action on ERα, G protein-coupled estrogen receptor (GPER) and the synthesis of 17β-estradiol (E2) were investigated using in vitro assays and molecular docking. The results showed that TPhP acted as an ERα agonist and recruited steroid receptor co-activator 1 (SRC1) and 3 (SRC3), which was found for the first time. Unlike TPhP, TDCIPP acted as an ERα antagonist. However, both TPhP and TDCIPP activated the estrogen pathway by GPER in SKBR3 cells which were lack of ERα. Although molecular docking results revealed that both TPhP and TDCIPP could dock into ERα and GPER, their substituent groups and combination mode might affect the receptor activation. In addition, by using estrogen biosynthesis assay in H295R cells, both of TPhP and TDCIPP were found to promote E2 synthesis and E2/T ratio involving their different alteration on levels of progesterone, testosterone and estrone, and expression of various key genes. Our data proposed estrogen-disrupting mechanism frameworks of TPhP and TDCIPP. Moreover, our results will contribute to future construction of adverse outcome pathway (AOP) framework of endocrine disruptors.
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| http://dx.doi.org/10.1016/j.ecoenv.2021.113069 | DOI Listing |
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