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大型溞暴露于亚致死剂量微囊藻毒素-LR后的慢性毒性及几种重要酶的反应

Chronic toxicity and responses of several important enzymes in Daphnia magna on exposure to sublethal microcystin-LR.

作者信息

Chen Wei, Song Lirong, Ou Danyun, Gan Nanqin

机构信息

State Key Laboratory of Freshwater Ecology and Biotechnology, Institute of Hydrobiology, Chinese Academy of Sciences, Wuhan, Hubei 430072, People's Republic of China.

出版信息

Environ Toxicol. 2005 Jun;20(3):323-30. doi: 10.1002/tox.20108.

Abstract

In the current study, the toxicological mechanisms of microcystin-LR and its disadvantageous effects on Daphnia magna were examined. Survival rate, number of newborn, activity of several important enzymes [glutathione S-transferase (GST), lactate dehydrogenase (LDH), phosphatases, and glutathione], accumulated microcystins, and ultrastructural changes in different organs of Daphnia were monitored over the course of 21-day chronic tests. The results indicated that low concentrations of dissolved microcystin had no harmful effect on Daphnia. On the contrary, stimulatory effects were detected. In the presence of toxin at high dosage and for long-term exposure, GST and glutathione levels decreased significantly. The decreased enzyme activity in the antioxidant system probably was caused by detoxification reactions with toxins. And these processes of detoxification at the beginning of chronic tests may enable phosphatases in Daphnia magna to withstand inhibition by the toxins. At the same time, we also found that the LDH activity in test animals increased with exposure to microcystin-LR, indicating that adverse effects occurred in Daphnia. With microcystin given at a higher dosage or for a longer exposure, the effect on Daphnia magna was fatal. In the meantime, microcystin began to accumulate in Daphnia magna, and phosphatase activity started to be inhibited. From the ultrastructure results of cells in D. magna, we obtained new information: the alimentary canal may be the target organ affected by exposure of microcystins to D. magna. The results of the current study also suggested that the oxidative damage and PPI (protein phosphatase inhibition) mechanisms of vertebrates also are adapted to Daphnia.

摘要

在本研究中,检测了微囊藻毒素-LR的毒理学机制及其对大型溞的不利影响。在为期21天的慢性试验过程中,监测了大型溞的存活率、新生个体数量、几种重要酶[谷胱甘肽S-转移酶(GST)、乳酸脱氢酶(LDH)、磷酸酶和谷胱甘肽]的活性、微囊藻毒素的积累情况以及不同器官的超微结构变化。结果表明,低浓度的溶解微囊藻毒素对大型溞没有有害影响。相反,检测到有刺激作用。在高剂量毒素长期存在的情况下,GST和谷胱甘肽水平显著下降。抗氧化系统中酶活性的降低可能是由与毒素的解毒反应引起的。而慢性试验开始时的这些解毒过程可能使大型溞中的磷酸酶能够抵抗毒素的抑制作用。同时,我们还发现试验动物体内的LDH活性随着微囊藻毒素-LR的暴露而增加,这表明大型溞出现了不良反应。给予较高剂量的微囊藻毒素或延长暴露时间,对大型溞的影响是致命的。与此同时,微囊藻毒素开始在大型溞中积累,磷酸酶活性开始受到抑制。从大型溞细胞的超微结构结果中,我们获得了新的信息:消化道可能是微囊藻毒素暴露影响大型溞的靶器官。本研究结果还表明,脊椎动物的氧化损伤和蛋白磷酸酶抑制(PPI)机制也适用于大型溞。

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