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Metabolism of Pyrene by the Aquatic Crustacean,Daphnia magna:Identification of Pyrene Metabolites and its Detoxification Enzymes

机译:水生甲壳动物的芘代谢,Daphnia magna:鉴定芘代谢物及其排毒酶

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The aquatic crustacean Daphnia magna is an important species for ecotoxicological study,and is often used as a test organism for environmental risk assessment.However,the mechanism of xenobiotic metabolism by this species has not been studied in detail.In the present study,pyrene was used as model substance to investigate the mechanism of xenobiotic metabolism in D.magna.The results of 24-h exposure experiments showed that D.magna could metabolize pyrene and biotransform it into water-soluble metabolites.On the other hand,the metabolism of pyrene was significantly inhibited by SKF-525A as the cytochrome P450(CYP)inhibitor.These observations indicated that oxidation by CYP participated in the biotransformation of pyrene by D.magna.We also identified the pyrene metabolites formed by D.magna by HPLC with an electrospray ionization triple quadrupole mass spectrometry detector(LC/ESI-MS/MS)and de-conjugation by sulfatase,beta-glucuronidase,and beta-glucosidase.One of the metabolites was ionized in ESI negative mode and formed a dominant mass of m/z 297(MS)with the product ion of m/z 217(MS~2).Furthermore,this metabolite formed 1-hydroxypyrene on treatment with sulfatase.This metabolite was considered to be a sulfate conjugate of oxidized pyrene(1-hydroxypyrene-sulfate).Furthermore,we quantified the deconjugated 1-hydroxypyrene formed by the above enzyme treatment.It showed that 52% of the total metabolized pyrene was biotransformed into 1-hydroxypyrene-sulfate,and more than 73% was biotransformed into oxidized pyrene conjugate.These results indicated that CYP and several conjugation enzymes participate in its biotransformation,and sulfation is important in D.magna for metabolism and elimination of xenobiotics.
机译:水生甲壳动物水蚤是生态毒理学研究中的一个重要品种,并经常被用来作为测试生物环境风险assessment.However,外源性代谢通过这一物种的机制还没有在detail.In进行研究本研究中,芘作为模型物质,调查表明,D.magna可代谢芘异生素代谢的在24小时暴露实验D.magna.The结果的机理和其生物转化成水溶性metabolites.On另一方面,芘的代谢SKF-525A作为细胞色素P450(CYP)抑制剂显着抑制。这些观察结果表明CYP的氧化参与了D.MAGNA的芘的生物转化。我们还通过HPLC用电喷雾鉴定了通过HPLC形成的芘代谢物电离三重四极杆质谱检测器(LC / ESI-MS / MS)和硫酸酶,β-葡糖醛酸糖苷酶和β-葡糖苷酶的去缀合物是代谢物的ION离子在ESI阴性模式下,用M / Z 217(MS〜2)的产物离子形成了M / Z 297(MS)的主要质量。许可,该代谢物形成1-羟基丙烯,用硫酸酶进行处理。认为代谢物作为氧化芘(1-羟基硫酸盐)的硫酸盐缀合物。加​​热,我们通过上述酶处理量化了DecoNupated 1-羟基丙烯。表明,52%的总代谢芘的生物转化为1-羟基硫酸盐并且超过73%的生物转化为氧化芘缀合物。结果表明CYP和几种共轭酶参与其生物转化,硫化在D.MAGNA中是重要的,用于代谢和消除异种症。

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