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Early zebrafish embryogenesis is susceptible to developmental TDCPP exposure

机译:斑马鱼早期胚胎发生易受TDCPP发育的影响

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Background: Chlorinated phosphate esters (CPEs) are widely used as additive flame retardants for low-density polyurethane foams and have frequently been detected at elevated concentrations within indoor environmental media. Objectives: To begin characterizing the potential toxicity of CPEs on early vertebrate development, we examined the developmental toxicity of four CPEs used in polyurethane foam: tris(1,3-dichloro-2-propyl) phosphate (TDCPP), tris(2-chloroethyl) phosphate (TCEP), tris(1-chloro-2-propyl) phosphate (TCPP), and 2,2-bis(chloromethyl)propane-1,3-diyl tetrakis(2-chlorethyl) bis(phosphate) (V6). Methods: Using zebrafish as a model for vertebrate embryogenesis, we first screened the potential teratogenic effects of TDCPP, TCEP, TCPP, and V6 using a developmental toxicity assay. Based on these results, we focused on identification of susceptible windows of developmental TDCPP exposure as well as evaluation of uptake and elimination of TDCPP and bis(1,3-dichloro-2-propyl)phosphate (BDCPP, the primary metabolite) within whole embryos. Finally, because TDCPP-specific genotoxicity assays have, for the most part, been negative in vivo and because zygotic genome remethylation is a key biological event during cleavage, we investigated whether TDCPP altered the status of zygotic genome methylation during early zebrafish embryogenesis. R esults: Overall, our findings suggest that the cleavage period during zebrafish embryogenesis is susceptible to TDCPP-induced delays in remethylation of the zygotic genome, a mechanism that may be associated with enhanced developmental toxicity following initiation of TDCPP exposure at the start of cleavage. C onclusions: Our results suggest that further research is needed to better understand the effects of a widely used and detected CPE within susceptible windows of early vertebrate development.
机译:背景:氯化磷酸酯(CPE)被广泛用作低密度聚氨酯泡沫的添加剂阻燃剂,并且经常在室内环境介质中以较高的浓度检测到。目的:为了开始表征CPE对脊椎动物早期发育的潜在毒性,我们研究了聚氨酯泡沫中使用的四种CPE的发育毒性:磷酸三(1,3-二氯-2-丙基)酯(TDCPP),磷酸三(2-氯乙基酯) )(TCEP),三(1-氯-2-丙基)磷酸(TCPP)和2,2-双(氯甲基)丙烷-1,3-二基四(2-氯乙基)双(磷酸盐)(V6) 。方法:使用斑马鱼作为脊椎动物胚胎发生的模型,我们首先使用发育毒性试验筛选了TDCPP,TCEP,TCPP和V6的潜在致畸作用。基于这些结果,我们专注于鉴定发育中的TDCPP暴露的敏感窗口,以及评估整个胚胎中TDCPP和双(1,3-二氯-2-丙基)磷酸酯(BDCPP,主要代谢产物)的摄取和消除。 。最后,由于TDCPP特异性遗传毒性测定在体内大部分是阴性的,并且由于合子基因组再甲基化是裂解过程中的关键生物学事件,因此我们研究了TDCPP是否在斑马鱼早期胚胎发生过程中改变了合子基因组甲基化的状态。结果:总体而言,我们的发现表明,斑马鱼胚胎发生过程中的卵裂期易受TDCPP诱导的合子基因组再甲基化延迟的影响,这种机制可能与卵裂开始时TDCPP暴露引发后发育毒性的增强有关。结论:我们的结果表明,需要进行进一步的研究以更好地了解在早期脊椎动物发育的易感窗口内广泛使用和检测到的CPE的影响。

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