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Developmental Toxicity of Diclofenac and Elucidation of Gene Regulation in zebrafish (Danio rerio)

机译:双氯芬酸的发育毒性和斑马鱼(Danio rerio)基因调控的阐明。

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摘要

Environmental pollution by emerging contaminants, e.g. pharmaceuticals, has become a matter of widespread concern in recent years. We investigated the membrane transport of diclofenac and its toxic effects on gene expression and the development of zebrafish embryos. The association of diclofenac with the embryos conformed to the general partition model at low concentration, the partition coefficient being 0.0033 ml per embryo. At high concentration, the interaction fitted the Freundlich model. Most of the diclofenac remained in the extracellular aqueous solution with less than 5% interacting with the embryo, about half of which was adsorbed on the membranes while the rest entered the cytoplasm. Concentrations of diclofenac over 10.13 μM were lethal to all the embryos, while 3.78 μM diclofenac was teratogenic. The development abnormalities at 4 day post treatment (dpt) include shorter body length, smaller eye, pericardial and body edema, lack of liver, intestine and circulation, muscle degeneration, and abnormal pigmentation. The portion of the diclofenac transferred into the embryo altered the expression of certain genes, e.g. down-regulation of Wnt3a and Gata4 and up-regulation of Wnt8a. The alteration of expression of such genes or the regulation of downstream genes could cause defects in the cardiovascular and nervous systems.
机译:新兴污染物对环境的污染,例如药物,近年来已成为广泛关注的问题。我们调查了双氯芬酸的膜运输及其对基因表达和斑马鱼胚胎发育的毒性作用。双氯芬酸与胚胎的缔合在低浓度时符合一般的分配模型,每个胚的分配系数为0.0033 ml。在高浓度下,相互作用符合Freundlich模型。大部分双氯芬酸保留在细胞外水溶液中,与胚胎的相互作用少于5%,其中约一半吸附在膜上,其余进入细胞质。双氯芬酸浓度超过10.13μM对所有胚胎致死,而3.78μmM双氯芬酸具有致畸性。治疗后第4天(dpt)的发育异常包括体长短,眼小,心包和身体浮肿,肝,肠和循环不足,肌肉变性和色素沉着异常。双氯芬酸转移到胚胎中的部分改变了某些基因的表达,例如。 Wnt3a和Gata4的下调和Wnt8a的上调。此类基因表达的改变或下游基因的调节可能导致心血管和神经系统的缺陷。

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