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维持组织中硒形态分布作为白鲟幼鱼抵御甲基汞毒性的潜在防御机制。

Maintaining tissue selenium species distribution as a potential defense mechanism against methylmercury toxicity in juvenile white sturgeon (Acipenser transmontanus).

机构信息

Centre for Advanced Research in Environmental Genomics, University of Ottawa, Ottawa, Ontario, Canada K1N 6N5.

Department of Animal Science, University of California, Davis, CA 95616, USA.

出版信息

Aquat Toxicol. 2014 Nov;156:88-95. doi: 10.1016/j.aquatox.2014.08.004. Epub 2014 Aug 17.

Abstract

Selenium (Se) has been shown to antagonize mercury (Hg) toxicity. We have previously demonstrated that orally intubated selenomethionine (SeMet) and methylmercury (MeHg) reduced tissue Se accumulation, as well as blood and kidney Hg concentrations in juvenile white sturgeon (Acipenser transmontanus). However, the form of Se accumulated is not known. In this study, three organoseleniums: selenocysteine (Sec), Se-methyl-selenocysteine (MSeCys), and SeMet and two inorganic Se species: selenate and selenite were determined and quantified in the blood at different post-intubation periods (12, 24, 48h) and in the muscle, liver, and kidneys at 48h in white sturgeon orally intubated with a single dose of control (carrier), SeMet (500μg Se/kg body weight; BW), MeHg (850μg Hg/kg BW), and both (Se+Hg; at 500μg Se/kg and 850μg Hg/kg BW). When only SeMet was intubated, the accumulative/unmodified pathway took precedent in the blood, white muscle, liver, and kidneys. In the presence of MeHg, however, active metabolic transformation and de novo synthesis of biologically active Se forms are seen in the liver and kidneys, as indicated by a gradual increase in blood Sec:SeMet ratios and Se metabolites. In the white muscle, mobilization of endogenous Se storage by MeHg is supported by the absence of tissue SeMet and detectable levels of blood SeMet. In contrast, co-intubation with SeMet increased muscle SeMet. The high levels of unknown Se metabolites and detectable levels of selenite in the kidney reflect its role as the major excretory organ for Se. Selenium metabolism is highly regulated in the kidneys, as Se speciation was not affected by MeHg or by its co-intubation with SeMet. In the Se+Hg group, the proportion of SeMet in the liver has decreased to nearly 1/8th of that of the SeMet only group, resulting in a more similar selenocompound distribution profile to that of the MeHg only group. This is likely due to the increased need for Se metabolites necessary for MeHg demethylation in the liver. Our study demonstrated that in the presence of MeHg, regulating tissue Se speciation, hence, Se bioavailability, is more an important strategy than maintaining total Se levels in major organs of juvenile white sturgeon.

摘要

硒(Se)已被证明能拮抗汞(Hg)的毒性。我们之前的研究表明,经口插管给予硒代蛋氨酸(SeMet)和甲基汞(MeHg)可减少幼年白鲟(Acipenser transmontanus)组织中的硒积累,以及血液和肾脏中的汞浓度。然而,积累的硒的形式尚不清楚。在这项研究中,三种有机硒化合物:硒代半胱氨酸(Sec)、硒甲基硒代半胱氨酸(MSeCys)和 SeMet,以及两种无机硒物种:硒酸盐和亚硒酸盐,在经口插管给予白鲟单一剂量的对照(载体)、SeMet(500μg Se/kg 体重;BW)、MeHg(850μg Hg/kg BW)和两者(Se+Hg;500μg Se/kg 和 850μg Hg/kg BW)后不同的插管后时期(12、24、48h)在血液中以及在 48h 时在肌肉、肝脏和肾脏中进行了测定和定量。当仅给予 SeMet 时,在血液、白肌肉、肝脏和肾脏中,累积/未修饰途径占主导地位。然而,在存在 MeHg 的情况下,肝脏和肾脏中可见到生物活性硒形式的主动代谢转化和从头合成,这表现为血液 Sec:SeMet 比值和硒代谢物逐渐增加。在白肌肉中,MeHg 动员内源性硒储存,这一点可由组织中没有 SeMet 和可检测到的血液 SeMet 水平得到支持。相比之下,与 SeMet 共同插管增加了肌肉中的 SeMet。肾脏中高浓度的未知硒代谢物和可检测到的亚硒酸盐反映了其作为硒主要排泄器官的作用。硒代谢在肾脏中受到高度调节,因为 MeHg 或与 SeMet 共同插管都没有影响硒的形态。在 Se+Hg 组中,肝脏中 SeMet 的比例已降至仅给予 SeMet 组的近 1/8,导致与仅给予 MeHg 组更相似的硒化合物分布谱。这可能是由于肝脏中需要更多用于 MeHg 去甲基化的硒代谢物所致。我们的研究表明,在存在 MeHg 的情况下,调节组织中的硒形态,从而调节硒的生物利用度,是比维持幼年白鲟主要器官中的总硒水平更重要的策略。

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