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6PPD 和 6PPD-醌在小鼠中的尿排泄、器官分布和胎盘转移及其通过核受体途径的潜在发育毒性。

Urine Excretion, Organ Distribution, and Placental Transfer of 6PPD and 6PPD-Quinone in Mice and Potential Developmental Toxicity through Nuclear Receptor Pathways.

机构信息

Skaggs School of Pharmacy and Pharmaceutical Sciences, University of California San Diego, La Jolla, California 92093, United States.

University of North Carolina Neuroscience Center, The University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599, United States.

出版信息

Environ Sci Technol. 2023 Sep 12;57(36):13429-13438. doi: 10.1021/acs.est.3c05026. Epub 2023 Aug 29.

Abstract

The rubber antioxidant 6PPD has gained significant attention due to its highly toxic transformation product, 6PPD-quinone (6PPDQ). Despite their detection in urines of pregnant women, the placental transfer and developmental toxicity of 6PPD and 6PPDQ are unknown. Here, we treated C57Bl/6 mice with 4 mg/kg 6PPD or 6PPDQ to investigate their urine excretion and placental transfer. Female and male mice exhibited sex difference in excretion profiles of 6PPD and 6PPDQ. Urine concentrations of 6PPDQ were one order of magnitude lower than those of 6PPD, suggesting lower excretion and higher bioaccumulation of 6PPDQ. In pregnant mice treated with 6PPD or 6PPDQ from embryonic day 11.5 to 15.5, 6PPDQ showed ∼1.5-8 times higher concentrations than 6PPD in placenta, embryo body, and embryo brain, suggesting higher placental transfer of 6PPDQ. Using in vitro dual-luciferase reporter assays, we revealed that 6PPDQ activated the human retinoic acid receptor α (RARα) and retinoid X receptor α (RXRα) at concentrations as low as 0.3 μM, which was ∼10-fold higher than the concentrations detected in human urines. 6PPD activated the RXRα at concentrations as low as 1.2 μM. These results demonstrate the exposure risks of 6PPD and 6PPDQ during pregnancy and emphasize the need for further toxicological and epidemiological investigations.

摘要

橡胶抗氧剂 6PPD 因其具有高毒性的转化产物 6PPD-醌(6PPDQ)而备受关注。尽管 6PPD 和 6PPDQ 已在孕妇尿液中被检测到,但它们在胎盘内的转移和发育毒性尚不清楚。在此,我们用 4mg/kg 的 6PPD 或 6PPDQ 处理 C57Bl/6 小鼠,以研究它们的尿液排泄和胎盘转移。雌性和雄性小鼠的 6PPD 和 6PPDQ 排泄特征存在性别差异。6PPDQ 的尿液浓度比 6PPD 低一个数量级,表明 6PPDQ 的排泄量较低,生物蓄积性较高。在从胚胎第 11.5 天至 15.5 天接受 6PPD 或 6PPDQ 处理的妊娠小鼠中,6PPDQ 在胎盘、胚胎体和胚胎脑中的浓度比 6PPD 高 1.5-8 倍,表明 6PPDQ 的胎盘转移较高。通过体外双荧光素酶报告基因检测,我们发现 6PPDQ 在低至 0.3μM 的浓度下即可激活人视黄酸受体 α(RARα)和视黄醇 X 受体 α(RXRα),这一浓度比在人尿液中检测到的浓度高 10 倍。6PPD 在低至 1.2μM 的浓度下即可激活 RXRα。这些结果表明在妊娠期间存在 6PPD 和 6PPDQ 的暴露风险,并强调需要进一步进行毒理学和流行病学研究。

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