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Induction of AhR transactivation by PBDD/Fs and PCDD/Fs using a novel human-relevant, high-throughput DR_(human) CALUX reporter gene assay

机译:使用新型人类相关,高通量DR_(人)CALUM报告基因测定的PBDD / FS和PCDD / FS对PBD / F和PCDD / FS的AHR转移诱导

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Polychlorinated dioxins and dibenzofurans (PCDD/Fs) are highly toxic contaminants that are strictly regulated and monitored in the environment and food to reduce human exposure. Recently, the increasing occurrence of polybrominated dioxins and dibenzofurans (PBDD/Fs) in the environment is raising concerns about the impact on human health by the combined exposure to chlorinated and brominated analogues of dioxins. Toxicological properties of PBDD/Fs relative to PCDD/Fs have not been firmly established, and brominated dioxins are not included in routine monitoring programs. In this study, we set out to determine human-relevant congener-specific potency values for a range of brominated and chlorinated dioxin congeners, based on their aryl hydrocarbon receptor (AhR)-mediated mode of toxic action. Transactivation of the AhR was measured using dioxin-responsive (DR) CALUX reporter gene assays. Because of known species-differences in dioxin-mediated toxicity, we developed and used a HepG2 human liver cell-based DR human CALUX assay that is a variant of the rodent-based DR CALUX. The assay was found to be highly inducible and stable, with low variations between independent measurements. Using both DR CALUX assays in an automated high-throughput mode we found that overall PBDD/Fs were as potent as PCDD/Fs in inducing AhR transactivation, but congener-specific differences were observed. We also observed species-specific differences in sensitivity and potency when comparing DR human REP values to those obtained in the rat-based DR CALUX. Finally, we observed significant differences between WHO-TEF values and DR human REP values, suggesting that actual WHO-TEF values may underestimate the hazards associated with exposure of humans to dioxins. (C) 2020 The Author(s). Published by Elsevier Ltd.
机译:多氯二恶英和二苯并呋喃(PCDD / FS)是毒性污染物,这些污染物受到环境和食物中严格调节和监测,以减少人体暴露。最近,在环境中增加了多溴二恶英和二苯并呋喃(PBDD / FS)的发生令人担忧对人类健康的影响通过联合暴露于二恶英的氯化和溴化类似物。 PBDD / FS相对于PCDD / FS的毒理学性质尚未牢固建立,并且溴化二恶英不包括在常规监测方案中。在这项研究中,我们首先基于其芳基烃受体(AHR)介导的毒性作用模式来确定一系列溴化和氯化二恶英同志仪的人文相关的Congener特异性效力值。使用二恶英响应(DR)CALUM报道器基因测定测量AHR的转移。由于已知的Dioxin介导的毒性差异,我们开发并使用了一种基于HepG2人肝细胞的DR人类阴卡测定,这是基于啮齿动物的CALUM的变体。发现测定是高度诱导和稳定的,在独立测量之间具有低变化。在自动化的高通量模式下使用DR CALUX测定,我们发现总体PBDD / FS作为诱导AHR转移激活的PCDD / FS是有效的,但观察到特异性差异。在将DR人Rep值与大鼠基于大鼠Calux中获得的那些中,我们还观察到敏感性和效力的物种特异性差异。最后,我们观察到WHO-TEF值与人类代价值之间的显着差异,表明实际的世卫组织值可能低估与二恶英暴露的危害。 (c)2020提交人。 elsevier有限公司出版

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