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首页> 外文期刊>Brain research >Protein kinase C is a target for diverse developmental neurotoxicants: transcriptional responses to chlorpyrifos, diazinon, dieldrin and divalent nickel in PC12 cells.
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Protein kinase C is a target for diverse developmental neurotoxicants: transcriptional responses to chlorpyrifos, diazinon, dieldrin and divalent nickel in PC12 cells.

机译:蛋白激酶C是多种发育性神经毒剂的靶标:PC12细胞中毒死rif,二嗪农,狄氏剂和二价镍的转录反应。

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Unrelated developmental neurotoxicants can elicit similar functional outcomes, whereas agents in the same class may differ. We compared two organophosphate insecticides (chlorpyrifos, diazinon) with an organochlorine (dieldrin) and a metal (Ni(2+)) for similarities and differences in their effects on gene expression encoding subtypes of protein kinase C and their modulators, a cell signaling cascade that integrates the actions of neurotrophic factors involved in brain development. We conducted evaluations in PC12 cells, a model for neuronal development, with each agent introduced at 30 microM for 24 or 72 h, treatments devoid of cytotoxicity. Chlorpyrifos evoked by far the largest effect, with widespread upregulation of multiple genes; the effects were greater during neurodifferentiation than when cells were exposed prior to differentiation. Diazinon had smaller and less widespread effects, consistent with its lesser long-term impact on synaptic function and behavior noted for in vivo exposures in developing rats. Surprisingly, the effects of diazinon, dieldrin and Ni(2+) showed basic similarities despite the fact that all three come from different classes of toxicants. Our findings provide some of the first evidence for a specific mechanistic cascade contributing to the cholinesterase-independent developmental neurotoxicant actions of chlorpyrifos and its differences from diazinon, while at the same time identifying mechanistic convergence between otherwise unrelated toxicants that provides predictions about common neurodevelopmental outcomes. These results further show how combined use of cell cultures and microarray technology can guide future in vivo work on diverse developmental neurotoxicants.
机译:无关的发育神经毒剂可以引起相似的功能结果,而同一类别的药物可能有所不同。我们比较了两种有机磷酸盐杀虫剂(毒死rif,二嗪农)与有机氯(狄氏剂)和金属(Ni(2+))的相似性和差异,它们对编码蛋白激酶C亚型的基因表达及其调节剂,细胞信号级联反应有影响整合了参与大脑发育的神经营养因子的作用。我们在PC12细胞(一种神经元发育模型)中进行了评估,每种药物以30 microM的剂量引入24或72 h,没有细胞毒性的治疗方法。毒死rif迄今为止引起的最大影响,是多种基因的广泛上调。与分化前暴露细胞相比,神经分化过程中的作用更大。二嗪农具有较小和较不广泛的作用,这与其在发育中大鼠体内暴露中对突触功能和行为的长期影响较小相一致。出乎意料的是,尽管所有这三种药物来自不同类别的毒物,但二嗪农,狄氏剂和Ni(2+)的作用显示出基本的相似性。我们的发现为特定机制的级联提供了一些初步证据,该机制有助于毒死rif的胆碱酯酶非依赖性发育神经毒性作用及其与二嗪农的区别,同时确定了其他无关的毒性物质之间的机制趋同,从而提供了对常见神经发育结果的预测。这些结果进一步表明,细胞培养与微阵列技术的结合使用如何指导未来在体内研究各种发育性神经毒性药物。

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