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Direct assessment of cumulative aryl hydrocarbon receptor agonist activity in sera from experimentally exposed mice and environmentally exposed humans

机译:直接评估实验暴露的小鼠和环境暴露的人血清中的累积芳基烃受体激动剂活性

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摘要

BACKGROUND: Aryl hydrocarbon receptor (AhR) ligands adversely affect many biological processes. However, assessment of the significance of human exposures is hampered by an incomplete understanding of how complex mixtures affect AhR activation/inactivation. OBJECTIVES: These studies used biological readouts to provide a broader context for estimating human risk than that obtained with serum extraction and gas chromatography/mass spectroscopy (GC/MS)-based assays alone. METHODS: AhR agonist activity was quantified in sera from dioxin-treated mice, commercial human sources, and polychlorinated biphenyl (PCB)-exposed Faroe Islanders using an AhR-driven reporter cell line. To validate relationships between serum AhR agonist levels and biological outcomes, AhR agonist activity in mouse sera correlated with toxic end points. AhR agonist activity in unmanipulated ("neat") human sera was compared with these biologically relevant doses and with GC/MS-assayed PCB levels. RESULTS: Mouse serum AhR agonist activity correlated with injected dioxin dose, thymic atrophy, and heptomegaly, validating the use of neat serum to assess AhR agonist activity. AhR agonist activity in sera from Faroe Islanders varied widely, was associated with the frequency of recent pilot whale dinners, but did not correlate with levels of PCBs quantified by GC/MS. Surprisingly, significant "baseline" AhR activity was found in commercial human sera. CONCLUSIONS: An AhR reporter assay revealed cumulative levels of AhR activation potential in neat serum, whereas extraction may preclude detection of important non-dioxin-like biological activity. Significant levels of AhR agonist activity in commercial sera and in Faroe Islander sera, compared with that from experimentally exposed mice, suggest human exposures that are biologically relevant in both populations.
机译:背景:芳烃受体(AhR)配体会对许多生物过程产生不利影响。但是,由于对复杂混合物如何影响AhR活化/失活的不完全了解,妨碍了对人类暴露影响的评估。目的:与仅基于血清提取和基于气相色谱/质谱(GC / MS)的分析相比,这些研究使用生物读数为估计人类风险提供了更广阔的背景。方法:使用AhR驱动的报告细胞系,对来自二恶英处理的小鼠,商业人源和暴露于多氯联苯(PCB)的法罗岛民的血清中的AhR激动剂活性进行了定量。为了验证血清AhR激动剂水平与生物学结果之间的关系,小鼠血清中的AhR激动剂活性与毒性终点相关。将未操作(“纯”)人血清中的AhR激动剂活性与这些生物学相关剂量以及GC / MS分析的PCB水平进行了比较。结果:小鼠血清AhR激动剂活性与注射的二恶英剂量,胸腺萎缩和肝肿大相关,验证了使用纯血清评估AhR激动剂活性。法罗群岛人血清中的AhR激动剂活性差异很大,与最近的飞行员鲸鱼晚餐的频率有关,但与通过GC / MS定量的PCBs水平无关。令人惊讶地,在商业人血清中发现了显着的“基线” AhR活性。结论:AhR报告基因检测揭示了纯血清中AhR激活潜能的累积水平,而提取可能排除了重要的非二恶英样生物活性的检测。与实验暴露的小鼠相比,商业血清和法罗岛民血清中的AhR激动剂活性水平显着升高,这表明这两种人群在生物学上均具有生物学意义。

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