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双酚类化合物和有机磷酸酯对 TM4 小鼠支持细胞影响的高内涵成像分析。

High-content imaging analyses of the effects of bisphenols and organophosphate esters on TM4 mouse Sertoli cells†.

机构信息

Department of Pharmacology and Therapeutics, McGill University, Montreal, Quebec, Canada.

Department of Obstetrics and Gynecology, McGill University, Montreal, Quebec, Canada.

出版信息

Biol Reprod. 2022 Sep 12;107(3):858-868. doi: 10.1093/biolre/ioac101.

Abstract

The endocrine disruptive effects of bisphenol A (BPA) and brominated flame retardants (BDE-47) have led to restrictions on their use and increased the pressure to identify safe replacements for these chemicals. Although there is evidence that some of these alternatives may be toxic to spermatogonial and Leydig cells, little is known about the toxicity of emerging replacements on Sertoli cells. We used high-content imaging to compare the effects of legacy chemicals, BPA and BDE-47, to their corresponding replacements. TM4 Sertoli cells were exposed for 48 h to each chemical (0.001-100 μM) followed by cytotoxicity and phenotypic endpoint assessment. The benchmark concentration potency ranking for bisphenols based on cytotoxicity was BPTMC > bisphenol M > BPAF>BPF > BPS > BPA. Human administered equivalent dose (AED) determination ranked BPS as the most potent alternative replacement. The benchmark concentration potency ranking of BDE-47 and organophosphate esters based on cytotoxicity was TDtBPP>BDMPP>TBOEP>TDCPP>TMPP>TPHP>BDE47>IPPP=BPDP=TCPP. Additionally, TM4 cell exposure to BDE-47 increased Calcein intensity (57.9 μM) and affected lysosomes (21.6 μM), while exposure to TPHP and TMPP resulted in cellular oxidative stress changes at benchmark concentration values as low as 0.01 and 0.4 μM, respectively. Overall bioactivity considerations of the chemicals on TM4 via ToxPi analyses and AED modeling further validated emerging replacements as highly potent chemicals in comparison to BPA and BDE-47. These findings demonstrate that many bisphenol and flame retardant replacements are more potent in Sertoli cells than the legacy chemical they are replacing and that phenotypic parameter assessment is an effective tool in chemical toxicity assessment.

摘要

双酚 A(BPA)和溴化阻燃剂(BDE-47)的内分泌干扰作用导致对它们的使用进行了限制,并增加了寻找这些化学物质安全替代品的压力。尽管有证据表明,其中一些替代品可能对精原细胞和莱迪希细胞有毒,但对于新兴替代品对支持细胞的毒性知之甚少。我们使用高内涵成像技术比较了传统化学物质 BPA 和 BDE-47 及其相应替代品的作用。TM4 支持细胞暴露于每种化学物质(0.001-100μM)48 小时,然后进行细胞毒性和表型终点评估。基于细胞毒性的双酚基准浓度效力排名为 BPTMC>BPAF>BPF> BPS> BPA。人类给药等效剂量(AED)测定将 BPS 列为最有效的替代替代品。基于细胞毒性的 BDE-47 和有机磷酸酯的基准浓度效力排名为 TDtBPP>BDMPP>TBOEP>TDCPP>TMPP>TPHP>BDE47>IPPP=BPDP=TCPP。此外,TM4 细胞暴露于 BDE-47 会增加钙黄绿素强度(57.9μM)并影响溶酶体(21.6μM),而 TPHP 和 TMPP 的暴露会导致细胞氧化应激变化,在基准浓度值低至 0.01 和 0.4μM 时分别如此。通过 ToxPi 分析和 AED 建模对 TM4 上化学物质的总体生物活性考虑进一步验证了新兴替代品与 BPA 和 BDE-47 相比是高度有效的化学物质。这些发现表明,许多双酚和阻燃剂替代品在支持细胞中的效力比它们所替代的传统化学物质更强,并且表型参数评估是化学毒性评估的有效工具。

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