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Effects of emerging contaminants on neurotransmission and biotransformation in marine organisms - An in vitro approach

机译:新兴污染物对海洋生物体内神经传递和生物转化的影响-体外方法

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The effects of gold (ionic form and nanopartides - AuNPs) and pharmaceuticals (carbamazepine and fluoxetine) on enzymes involved in neurotransmission (acetylcholinesterase - AChE) and biotransformation (glutathione S-transferases - GST) were assessed by their incubation with Mytilus galloprovincialis' hemolymph and subcellular fraction of gills, respectively. AuNPs did not alter enzymatic activities unlike ionic gold that inhibited AChE and GST activities at 2.5 and 0.42 mg.L-1, respectively. Carbamazepine inhibited AChE activity at 500 mg.L-1 and fluoxetine at 1000 mg.L-1. GST was inhibited by carbamazepine at 250 mg.L-1 and by fluoxetine at 125 mg.L-1. Increased AChE activity was found in simultaneous exposures to fluoxetine and bovine serum albumin coated AuNPs (BSA-AuNPs). Concerning GST, in the simultaneous exposures, AuNPs revealed protective effects against carbamazepine (citrate and polyvinylpyrrolidone coated) and fluoxetine (citrate and BSA coated) induced inhibition. However, BSA-AuNPs increased the inhibition caused by carbamazepine. AuNPs demonstrated ability to interfere with other chemicals toxicity justifying further studies. (C) 2016 Elsevier Ltd. All rights reserved.
机译:通过将金(离子形式和纳米粒子-AuNPs)和药物(卡马西平和氟西汀)与神经传递(乙酰胆碱酯酶-AChE)和生物转化(谷胱甘肽S-转移酶-GST)有关的酶与金芽孢杆菌(Mytilus galloprovincialis)的血淋巴液一起温育,评估了它们的作用。 cellular的亚细胞部分。 AuNPs不会改变酶活性,这与离子金分别抑制AChE和GST活性分别在2.5和0.42 mg.L-1上有关。卡马西平在500 mg.L-1时抑制AChE活性,在1000 mg.L-1时抑制氟西汀。 250 mg.L-1的卡马西平和125 mg.L-1的氟西汀抑制GST。在同时暴露于氟西汀和牛血清白蛋白包被的AuNPs(BSA-AuNPs)中,发现AChE活性增加。关于GST,在同时暴露中,AuNPs表现出对卡马西平(柠檬酸盐和聚乙烯吡咯烷酮涂层)和氟西汀(柠檬酸盐和BSA涂层)诱导的抑制作用的保护作用。但是,BSA-AuNPs增加了卡马西平引起的抑制作用。 AuNPs具有干扰其他化学物质毒性的能力,因此有待进一步研究。 (C)2016 Elsevier Ltd.保留所有权利。

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