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首页> 外文期刊>Environmental health perspectives. >Polybrominated Diphenyl Ethers Induce Developmental Neurotoxicity in a Human in Vitro Model: Evidence for Endocrine Disruption
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Polybrominated Diphenyl Ethers Induce Developmental Neurotoxicity in a Human in Vitro Model: Evidence for Endocrine Disruption

机译:多溴联苯醚在人类体外模型中诱导发育性神经毒性:内分泌干扰的证据

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摘要

Background Polybrominated diphenyl ethers (PBDEs) are persistent and bioaccumulative flame retardants, which are found in rising concentrations in human tissues. They are of concern for human health because animal studies have shown that they possess the potential to be developmentally neurotoxic. Objective Because there is little knowledge of the effects of PBDEs on human brain cells, we investigated their toxic potential for human neural development in vitro . Moreover, we studied the involvement of thyroid hormone (TH) disruption in the effects caused by PBDEs. Methods We used the two PBDE congeners BDE-47 and BDE-99 (0.1–10 μM), which are most prominent in human tissues. As a model of neural development, we employed primary fetal human neural progenitor cells (hNPCs), which are cultured as neurospheres and mimic basic processes of brain development in vitro : proliferation, migration, and differentiation. Results PBDEs do not disturb hNPC proliferation but decrease migration distance of hNPCs. Moreover, they cause a reduction of differentiation into neurons and oligodendrocytes. Simultaneous exposure with the TH receptor (THR) agonist triiodothyronine rescues these effects on migration and differentiation, whereas the THR antagonist NH-3 does not exert an additive effect. Conclusion PBDEs disturb development of hNPCs in vitro via endocrine disruption of cellular TH signaling at concentrations that might be of relevance for human exposure.
机译:背景技术多溴二苯醚(PBDEs)是持久性和生物蓄积性阻燃剂,在人体组织中的浓度不断升高。它们对人类健康至关重要,因为动物研究表明它们具有发展神经毒性的潜力。目的由于对多溴二苯醚对人脑细胞的作用了解甚少,因此我们研究了其对体外人神经发育的潜在毒性。此外,我们研究了多溴二苯醚对甲状腺激素(TH)破坏的影响。方法我们使用了两种PBDE同源物BDE-47和BDE-99(0.1–10μM),它们在人体组织中最为突出。作为神经发育的模型,我们采用了原代胎儿人类神经祖细胞(hNPC),将其培养为神经球并模仿体外脑发育的基本过程:增殖,迁移和分化。结果PBDEs不会干扰hNPC的增殖,但会减少hNPC的迁移距离。而且,它们引起分化为神经元和少突胶质细胞的减少。与TH受体(THR)激动剂三碘甲甲状腺素同时暴露可挽救这些对迁移和分化的影响,而THR拮抗剂NH-3则不发挥累加作用。结论PBDEs可能通过内分泌干扰细胞TH信号传导而干扰hNPC的体外发育,其浓度可能与人体暴露有关。

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