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全氟烷基和多氟烷基物质二元组合在 FaO 细胞中的转录效应。

Transcriptional effects of binary combinations of PFAS in FaO cells.

作者信息

Bjork James A, Dawson Douglas A, Krogstad Jacob O, Wallace Kendall B

机构信息

University of Minnesota Medical School, Department of Biomedical Sciences, 1035 University Drive, Duluth, MN, 55812, United States.

Department of Biology/Toxicology, 318 Kettering Science Center, Ashland University, Ashland, OH, United States.

出版信息

Toxicology. 2021 Dec;464:152997. doi: 10.1016/j.tox.2021.152997. Epub 2021 Oct 22.

Abstract

Per- and polyfluoroalkyl substances (PFAS) represent a large class of structurally diverse chemicals of increasing public concern, mostly due to their chemical stability and undetermined toxicity profiles. In laboratory animals, adverse effects implicated for certain PFAS, perfluorooctanoic acid (PFOA) and perfluorooctane sulfonate (PFOS) in particular, include liver toxicity and the associated metabolic dysregulation, immune and thyroid alterations, reproductive toxicity, and selected tumors. The broad commercialization and environmental distribution of PFAS has drawn attention to the need for understanding risks associated with combined exposure to multiple PFAS in complex mixtures. The purpose of this investigation is to determine whether binary combinations of PFAS elicit a molecular response that is either greater than or less than the sum of the individual responses. Exposure of FaO rat hepatoma cells for 24 h to 25 μM-200 μM of the 4- and 8-carbon perfluorocarboxylic acids (PFBA and PFOA) or the 4, 6, and 8-carbon perfluorosulfonic acids (PFBS, PFHxS, and PFOS, respectively) individually caused a dose-dependent increase in PPARα-regulated expression of peroxisomal bifunctional enzyme (Ehhadh). Potency increased with carbon number, with the carboxylates eliciting a greater transcriptional response than the corresponding sulfonates. Combined exposure to PFOA and PFBA produced an effect that was significantly less than the sum of the individual responses. The response to the combination of PFOA and PFOS produced a summative effect at concentrations that were not cytotoxic. Combined exposures to PFOS and either PFBS or PFHxS at low noncytotoxic concentrations produced a transcriptional effect that was significantly less than the sum of the individual effects. The results demonstrate that among the five structurally related perfluoroalkyl acids included in this investigation, PPARα transcriptional activation in response to combined binary exposures is consistently at or below that predicted by the sum of the individual effects.

摘要

全氟和多氟烷基物质(PFAS)是一大类结构多样的化学物质,日益引起公众关注,主要是因为它们的化学稳定性和尚未确定的毒性特征。在实验动物中,某些PFAS,特别是全氟辛酸(PFOA)和全氟辛烷磺酸(PFOS)的不良反应包括肝脏毒性及相关的代谢失调、免疫和甲状腺改变、生殖毒性以及特定肿瘤。PFAS的广泛商业化和环境分布已引起人们对了解复杂混合物中多种PFAS联合暴露相关风险的关注。本研究的目的是确定PFAS的二元组合是否会引发大于或小于个体反应总和的分子反应。将FaO大鼠肝癌细胞暴露于25μM至200μM的4碳和8碳全氟羧酸(PFBA和PFOA)或4碳、6碳和8碳全氟磺酸(分别为PFBS、PFHxS和PFOS)中24小时,单独暴露会导致过氧化物酶体双功能酶(Ehhadh)的PPARα调节表达呈剂量依赖性增加。效力随碳原子数增加,羧酸盐引发的转录反应比相应的磺酸盐更大。PFOA和PFBA联合暴露产生的效应明显小于个体反应之和。在无细胞毒性的浓度下,对PFOA和PFOS组合的反应产生了累加效应。在低无细胞毒性浓度下,PFOS与PFBS或PFHxS联合暴露产生的转录效应明显小于个体效应之和。结果表明,在本研究中包含的五种结构相关的全氟烷基酸中,对二元联合暴露的PPARα转录激活始终等于或低于个体效应之和所预测的值。

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