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Hepatic CYP1A induction by dioxin-like compounds, and congener-specific metabolism and sequestration in wild common cormorants from Lake Biwa, Japan

机译:二恶英类化合物诱导肝脏CYP1A的代谢,以及来自日本琵琶湖的野生普通cor的同族物特异性代谢和螯合

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The present study examines the effects of polychlorinated dibenzo-p-dioxins (PCDDs), polychlorinated dibenzofurans (PCDFs), and coplanar polychlorinated biphenyls (Co-PCBs) on hepatic cytochromes P450 (CYP) in the wild population of common cormorants from Lake Biwa, Japan, and discusses functional roles of CYP1A in terms of correlation analysis between tissue concentrations of individual congeners and expression levels of CYP1A. Levels of alkoxyresorufin (methoxy-, ethoxy-, pentoxy-, and benzyloxyresorufin) O-dealkylase activities and a protein cross-reacted with anti-rat CYP1A1 polyclonal antibodies showed significant positive correlations with total 2,3,7,8-tetra chlorodibenzo-p-dioxin toxic equivalents (TEQs) or TEQs for most individual congeners in the liver of cormorants, suggesting induction of CYP1A-like protein by these chemicals. In contrast, TEQs for lower chlorinated congeners, 2,3,7,8-T4CDF and PCB77, showed relatively low correlations with the expression level of CYP1A-like protein. Concentrations of 2,3,7,8-T4CDF and PCB77 normalized to a relatively recalcitrant congener, PCB169, were negatively correlated with the CYP1A-like protein level. These results indicate preferential metabolism of those congeners by CYP1A-like protein that was induced by TEQs. Concentration ratios of liver to pectoral muscle for certain congeners significantly increased with an elevation of the CYP1A-like protein level. Comparing the results in the present study with those of previous studies using rodents treated with certain dioxin-like congeners, these congeners in the liver may be sequestered by CYP1A. Levels of cross-reactive proteins with anti-rat CYP2B1, CYP2C6, and CYP3A2 polyclonal antibodies correlated with neither TEQs nor liver/muscle concentration ratios of congeners. We conclude that the potential for CYP1A induction, and metabolism and sequestration of dioxin-like compounds by CYP1A, may be a critical factor for assessing the ecological risk in wild avian species.
机译:本研究调查了来自琵琶湖常见cor野生种群中多氯二苯并对二恶英(PCDD),多氯二苯并呋喃(PCDF)和共平面多氯联苯(Co-PCBs)对肝细胞色素P450(CYP)的影响,日本,并讨论了CYP1A的功能作用,涉及各个同源物的组织浓度与CYP1A的表达水平之间的相关性分析。烷氧基间苯二酚(甲氧基,乙氧基,戊氧基和苄氧基间苯二酚)的O-脱烷基酶活性以及与抗大鼠CYP1A1多克隆抗体交叉反应的蛋白质显示与总的2,3,7,8-四氯二苯并-正相关-肝脏中大多数个体同源物的对二恶英毒性当量(TEQs)或TEQ,表明这些化学物质可诱导CYP1A样蛋白的生成。相比之下,较低的氯化同类物,2、3、7、8-T4CDF和PCB77的TEQ与CYP1A样蛋白的表达水平相关性较低。归一化为相对顽固同源物PCB169的2,3,7,8-T4CDF和PCB77的浓度与CYP1A样蛋白水平呈负相关。这些结果表明由TEQs诱导的CYP1A样蛋白优先代谢这些同类物。某些同类物的肝脏与胸肌的浓度比随着CYP1A样蛋白水平的升高而显着增加。将本研究的结果与使用某些二恶英样同源物治疗的啮齿类动物的先前研究结果进行比较,肝脏中的这些同源物可能被CYP1A隔离。具有抗大鼠CYP2B1,CYP2C6和CYP3A2多克隆抗体的交叉反应蛋白的水平与TEQ或同类物的肝/肌肉浓度比均不相关。我们得出的结论是,潜在的CYP1A诱导作用,以及CYP1A对二恶英样化合物的代谢和隔离可能是评估野生鸟类生态风险的关键因素。

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