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生成荧光斑马鱼研究内分泌干扰和甲状腺激素与皮质类固醇之间的潜在串扰。

Generation of fluorescent zebrafish to study endocrine disruption and potential crosstalk between thyroid hormone and corticosteroids.

机构信息

INRA UR 1037 SCRIBE, IFR 140, 35042 Rennes Cedex, France.

出版信息

Aquat Toxicol. 2011 Sep;105(1-2):13-20. doi: 10.1016/j.aquatox.2011.04.007. Epub 2011 May 27.

Abstract

Several environmental chemicals disrupt thyroid function, a key regulator of normal development involved in many physiological processes in fish. We studied the effects of such chemicals in vivo using transient transgenic zebrafish (Danio rerio), expressing Green Fluorescent Protein (GFP) under the control of a TH/bZIP promoter from Xenopus laevis. Exposure to thyroid hormone (T3) at 10(-8)M increased GFP fluorescence in F0 embryos and larvae. Transient transgenic embryos were exposed to a T3 signaling agonist (TRIAC) or antagonists (NH(3) or NaClO(4)), or to the endocrine disruptor Bisphenol A (BPA). When tested alone, TRIAC increased fluorescence, confirming the specificity of our model. Exposure to NH(3) or NaClO(4) decreased fluorescence, reflecting inhibition of thyroid function. When tested alone, BPA did not modify fluorescence, but when tested with T3, it significantly reduced T3-induced fluorescence, suggesting disruption of the thyroid function by BPA. The expression of genes involved in the TH axis (TR-alpha, TR-beta, TSH) and the corticoid axis (GR and MR) was followed by q-PCR after T3 or BPA exposure (24 or 48h) and at different developmental stages (0, 1, or 5 days post-fertilization). Expression of TR-alpha, TR-beta, and TSH genes increased after 48h T3 exposure in 1-day-old larvae. When tested alone, BPA only slightly affected gene expression. When applied with T3, BPA decreased expression of all candidate genes in 1-day-old embryos compared to the T3 treated group, in agreement with data obtained with the TH/bZIP-eGFP zebrafish model. Finally, we show that T3 exposure leads to up-regulation of MR and GR genes. This study provides a new rapid diagnostic tool for characterizing the disrupting effects of toxicants on thyroid function and suggests possible crosstalk between the TR and Corticoid Signaling system.

摘要

几种环境化学物质会干扰甲状腺功能,甲状腺是鱼类许多生理过程中正常发育的关键调节剂。我们使用瞬时转基因斑马鱼(Danio rerio)在体内研究了这些化学物质的影响,该鱼的 GFP 在非洲爪蟾的 TH/bZIP 启动子的控制下表达。在 10(-8)M 的甲状腺激素 (T3) 暴露下,F0 胚胎和幼虫的 GFP 荧光增加。瞬时转基因胚胎暴露于 T3 信号激动剂 (TRIAC) 或拮抗剂 (NH(3) 或 NaClO(4)) 或内分泌干扰物双酚 A (BPA) 中。单独测试时,TRIAC 增加了荧光,证实了我们模型的特异性。暴露于 NH(3) 或 NaClO(4) 降低了荧光,反映了甲状腺功能的抑制。单独测试时,BPA 不会改变荧光,但与 T3 一起测试时,它显著降低了 T3 诱导的荧光,表明 BPA 对甲状腺功能的破坏。在 T3 或 BPA 暴露(24 或 48 小时)后和不同发育阶段(受精后 0、1 或 5 天),通过 q-PCR 检测参与 TH 轴(TR-alpha、TR-beta、TSH)和皮质激素轴(GR 和 MR)的基因表达。在 1 天龄幼虫中,在 48 小时 T3 暴露后,TR-alpha、TR-beta 和 TSH 基因的表达增加。单独测试时,BPA 仅轻微影响基因表达。当与 T3 一起应用时,BPA 与 T3 处理组相比,在 1 天龄胚胎中降低了所有候选基因的表达,这与使用 TH/bZIP-eGFP 斑马鱼模型获得的数据一致。最后,我们发现 T3 暴露会导致 MR 和 GR 基因的上调。这项研究提供了一种新的快速诊断工具,用于描述有毒物质对甲状腺功能的破坏作用,并表明 TR 和皮质激素信号系统之间可能存在串扰。

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