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首页> 外文期刊>Environmental health perspectives. >Serum Metabolomic Profiles in Neonatal Mice following Oral Brominated Flame Retardant Exposures to Hexabromocyclododecane (HBCD) Alpha, Gamma, and Commercial Mixture
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Serum Metabolomic Profiles in Neonatal Mice following Oral Brominated Flame Retardant Exposures to Hexabromocyclododecane (HBCD) Alpha, Gamma, and Commercial Mixture

机译:口服溴化阻燃剂暴露于六溴环十二烷(HBCD)α,γ和商业混合物后,新生小鼠的血清代谢组学特征

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Background: Hexabromocyclododecane (HBCD) is a high production volume brominated flame retardant added to building insulation foams, electronics, and textiles. HBCD is a commercial mixture (CM-HBCD) composed of three main stereoisomers: α-HBCD (10%), β-HBCD (10%), and γ-HBCD (80%). A shift from the dominant stereoisomer γ-HBCD to α-HBCD is detected in humans and wildlife. Objectives: Considering CM-HBCD has been implicated in neurodevelopment and endocrine disruption, with expected metabolism perturbations, we performed metabolomics on mice serum obtained during a window-of-developmental neurotoxicity to draw correlations between early-life exposures and developmental outcomes and to predict health risks. Methods: Six female C57BL/6 mice at postnatal day (PND) 10 were administered a single gavage dose of α-, γ-, or CM-HBCD at 3, 10, and 30 mg/kg. Nuclear magnetic resonance metabolomics was used to analyze 60 μL serum aliquots of blood collected 4 days post-oral exposure. Results: Infantile mice exposed to α-, γ-, or CM-HBCD demonstrated differences in endogenous metabolites by treatment and dose groups, including metabolites involved in glycolysis, gluconeogenesis, lipid metabolism, citric acid cycle, and neurodevelopment. Ketone bodies, 3-hydroxybutyrate, and acetoacetate, were nonstatistically elevated, when compared with mean control levels, in all treatment and dose groups, while glucose, pyruvate, and alanine varied. Acetoacetate was significantly increased in the 10 mg/kg α-HBCD and was nonsignificantly decreased with CM-HBCD. A third ketone body, acetone, was significantly lower in the 30 mg/kg α-HBCD group with significant increases in pyruvate at the same treatment and dose group. Metabolites significant in differentiating treatment and dose groups were also identified, including decreases in amino acids glutamate (excitatory neurotransmitter in learning and memory) and phenylalanine (neurotransmitter precursor) after α-HBCD and γ-HBCD exposure, respectively. Conclusions: We demonstrated that 4 days following a single neonatal oral exposure to α-, γ-, and CM-HBCD resulted in different serum metabolomic profiles, indicating stereoisomer- and mixture-specific effects and possible mechanisms of action. Citation: Szabo DT, Pathmasiri W, Sumner S, Birnbaum LS. 2017. Serum metabolomic profiles in neonatal mice following oral brominated flame retardant exposures to hexabromocyclododecane (HBCD) alpha, gamma, and commercial mixture. Environ Health Perspect 125:651–659; http://dx.doi.org/10.1289/EHP242.
机译:背景:六溴环十二烷(HBCD)是一种高产量的溴化阻燃剂,已添加到建筑保温泡沫,电子产品和纺织品中。六溴环十二烷是一种商业混合物(CM-HBCD),由三种主要的立体异构体组成:α-六溴环十二烷(10%),β-六溴环十二烷(10%)和γ-六溴环十二烷(80%)。在人类和野生生物中检测到从主要的立体异构体γ-HBCD转变为α-HBCD。目的:考虑到CM-HBCD已参与神经发育和内分泌破坏,并伴随预期的代谢紊乱,我们对在发育窗口神经毒性过程中获得的小鼠血清进行了代谢组学研究,以得出早期暴露与发育结果之间的相关性并预测健康风险。方法:六只雌性C57BL / 6小鼠在出生后第10天(PND)分别以3、10和30 mg / kg的剂量单独饲喂α-,γ-或CM-HBCD。核磁共振代谢组学用于分析口服暴露后4天收集的60μL血液的等分试样。结果:暴露于α-,γ-或CM-HBCD的婴儿小鼠按治疗和剂量组显示内源性代谢物的差异,包括参与糖酵解,糖异生,脂质代谢,柠檬酸循环和神经发育的代谢物。与平均对照组相比,在所有治疗和剂量组中,酮体(3-羟基丁酸酯和乙酰乙酸酯)均未统计升高,而葡萄糖,丙酮酸和丙氨酸则有所变化。在10 mg / kgα-六溴环十二烷中,乙酰乙酸酯显着增加,而在CM-六溴环十二烷中,乙酰乙酸酯无明显下降。在30 mg / kg的α-六溴环十二烷组中,第三个酮体丙酮显着降低,而在相同的治疗和剂量组中丙酮酸显着增加。还确定了在区分治疗和剂量组方面有重要意义的代谢物,包括分别暴露于α-HBCD和γ-HBCD之后的谷氨酸(学习和记忆中的兴奋性神经递质)和苯丙氨酸(神经递质前体)减少。结论:我们证明,单次新生儿口服α-,γ-和CM-HBCD后4天会导致不同的血清代谢组学特征,表明立体异构体和混合物特异性作用以及可能的作用机制。引文:Szabo DT,Pathmasiri W,Sumner S,Birnbaum LS。 2017。口服溴化阻燃剂暴露于六溴环十二烷(HBCD)α,γ和商业混合物后,新生小鼠的血清代谢组学特征。环境健康透视125:651–659; http://dx.doi.org/10.1289/EHP242。

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