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Can profiles of poly- and Perfluoroalkyl substances (PFASs) in human serum provide information on major exposure sources?

机译:人体血清中的聚 - 和全氟烷基物质(PFASS)的谱提供有关主要曝光源的信息吗?

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摘要

Abstract Background Humans are exposed to poly- and perfluoroalkyl substances (PFASs) from diverse sources and this has been associated with negative health impacts. Advances in analytical methods have enabled routine detection of more than 15 PFASs in human sera, allowing better profiling of PFAS exposures. The composition of PFASs in human sera reflects the complexity of exposure sources but source identification can be confounded by differences in toxicokinetics affecting uptake, distribution, and elimination. Common PFASs, such as perfluorooctanoic acid (PFOA), perfluorooctane sulfonic acid (PFOS) and their precursors are ubiquitous in multiple exposure sources. However, their composition varies among sources, which may impact associated adverse health effects. Methods We use available PFAS concentrations from several demographic groups in a North Atlantic seafood consuming population (Faroe Islands) to explore whether chemical fingerprints in human sera provide insights into predominant exposure sources. We compare serum PFAS profiles from Faroese individuals to other North American populations to investigate commonalities in potential exposure sources. We compare individuals with similar demographic and physiological characteristics and samples from the same years to reduce confounding by toxicokinetic differences and changing environmental releases. Results Using principal components analysis (PCA) confirmed by hierarchical clustering, we assess variability in serum PFAS concentrations across three Faroese groups. The first principal component (PC)/cluster consists of C9-C12 perfluoroalkyl carboxylates (PFCAs) and is consistent with measured PFAS profiles in consumed seafood. The second PC/cluster includes perfluorohexanesulfonic acid (PFHxS) and the PFOS precursor N-ethyl perfluorooctane sulfonamidoacetate (N-EtFOSAA), which are directly used or metabolized from fluorochemicals in consumer products such as carpet and food packaging. We find that the same compounds are associated with the same exposure sources in two North American populations, suggesting generalizability of results from the Faroese population. Conclusions We conclude that PFAS homologue profiles in serum provide valuable information on major exposure sources. It is essential to compare samples collected at similar time periods and to correct for demographic groups that are highly affected by differences in physiological processes (e.g., pregnancy). Information on PFAS homologue profiles is crucial for attributing adverse health effects to the proper mixtures or individual PFASs.
机译:摘要背景人类受到不同来源的多氟烷基物质(PFASS),这与负面健康影响有关。分析方法的进步使得人血清中的常规检测超过15个PFASS,允许PFAS曝光的更好分析。人血清中PFASS的组成反映了暴露源的复杂性,但可以通过影响摄取,分布和消除的毒物动脉学的差异来混淆来源鉴定。常见的PFASS,如全氟辛酸(PFOA),全氟辛烷磺酸(PFOS)及其前体在多种曝光源中普遍存在。然而,它们的组成在来源之间变化,可能影响相关的不良健康影响。方法我们使用北大西洋海产品消费人口(法罗群岛)的几个人口统计集团的可用PFA浓度来探索人类血清中的化学指纹是否能够进入主要的暴露来源。我们比较Faroese个人的血清PFAS档案到其他北美人群,以调查潜在暴露来源的共性。我们比较具有相同年份的人口和生理特性和样品的个体,以减少毒物动力学差异和改变环境释放的混淆。结果采用分层聚类证实的主要成分分析(PCA),我们评估了三个Faroese群体血清PFA浓度的可变性。第一主成分(PC)/簇由C9-C12全氟烷基羧酸盐(PFCAs)组成,并与在消耗的海鲜中测量的PFAS曲线一致。第二个PC /簇包括全氟己酸磺酸(PFHX)和PFOS前体N-乙基全氟辛酸磺胺酰胺(N-ETFOSA),其直接从消费品和食品包装等消费产品中的含氟化合物使用或代谢。我们发现相同的化合物与两名北美人群的相同曝光来源有关,表明Faroese人口的概括性。结论我们得出结论,血清中的PFAS同源物谱提供了关于主要曝光来源的有价值的信息。必须将在类似时间段收集的样本进行比较,并纠正受到生理过程差异影响的人口统计学组(例如,怀孕)。关于PFAS同源物型材的信息对于将对适当的混合物或单个PFASS归因于适当的混合物或单独的PFASS来说至关重要。

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