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首页> 外文期刊>Drug Metabolism and Disposition: The Biological Fate of Chemicals >Tissue-specific metabolism of benzo[a]pyrene in rainbow trout (oncorhynchus mykiss): A comparison between the liver and immune organs
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Tissue-specific metabolism of benzo[a]pyrene in rainbow trout (oncorhynchus mykiss): A comparison between the liver and immune organs

机译:虹鳟鱼(oncorhynchus mykiss)中苯并[a] py的组织特异性代谢:肝脏与免疫器官的比较

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Polycyclic aromatic hydrocarbons (PAHs) are immunotoxicants in fish. In mammals, phase I metabolites are believed to be critically involved in the immunotoxicity of PAHs. This mechanism has been suggested for fish as well. The present study investigates the capacity of immune organs (head kidney, spleen) of rainbow trout, Oncorhynchus mykiss, to metabolize the prototypic PAH, benzo [a]pyrene (BaP). To this end, we analyzed 1) the induction of enzymatic capacity measured as 7-ethoxyresorufin-O-deethylase (EROD) activity in immune organs compared with liver, 2) the organ profiles of BaP metabolites generated in vivo, and 3) rates of microsomal BaP metabolite production in vitro. All measurements were done for control fish and for fish treated with an intraperitoneal injection of 15 mg BaP/kg body weight. In exposed trout, the liver, head kidney, and spleen contained similar levels of BaP, whereas EROD induction differed significantly between the organs, with liver showing the highest induction factor (132.8×), followed by head kidney (38.4×) and spleen (1.4×). Likewise, rates of microsomal metabolite formation experienced the highest induction in the liver of BaP-exposed trout, followed by the head kidney and spleen. Microsomes from control fish displayed tissue-specific differences in metabolite production. In contrast, in BaP-exposed trout, microsomes of all organs produced the potentially immunotoxic BaP-7,8-dihydrodiol as the main metabolite. The findings from this study show that PAHs, like BaP, are distributed into immune organs of fish and provide the first evidence that immune organs possess inducible PAH metabolism leading to in situ production of potentially immunotoxic PAH metabolites.
机译:多环芳烃(PAHs)是鱼类中的免疫毒性物质。在哺乳动物中,I期代谢产物被认为与PAHs的免疫毒性至关重要。有人还建议将这种机制用于鱼类。本研究调查了虹鳟鱼Onmyhynchus mykiss的免疫器官(头肾,脾脏)代谢原型PAH,苯并[a]((BaP)的能力。为此,我们分析了1)与肝脏相比,在免疫器官中诱导为7-乙氧基间苯二酚-O-脱乙基酶(EROD)活性的酶促能力; 2)体内产生的BaP代谢物的器官特征,以及3)体外微粒体BaP代谢产物的产生。对对照鱼和腹膜内注射15 mg BaP / kg体重的鱼进行所有测量。在裸露的鳟鱼中,肝,头肾和脾脏的BaP含量相似,而器官间的EROD诱导差异显着,肝脏的诱导因子最高(132.8x),其次是头肾(38.4x)和脾脏(38.4x)。 1.4倍)。同样,微粒体代谢物形成的速率在暴露于BaP的鳟鱼的肝脏中经历了最高的诱导,其次是头部肾脏和脾脏。对照鱼的微粒体在代谢产物产生中表现出组织特异性差异。相反,在暴露于BaP的鳟鱼中,所有器官的微粒体均会产生潜在的免疫毒性BaP-7,8-二氢二醇作为主要代谢产物。这项研究的发现表明,PAHs与BaP一样分布在鱼类的免疫器官中,并提供了第一个证据,表明免疫器官具有可诱导的PAH代谢,从而导致原位产生潜在的免疫毒性PAH代谢产物。

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