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美国卡车运输业中与交通相关的污染物暴露的综合分子反应。

Integrated molecular response of exposure to traffic-related pollutants in the US trucking industry.

机构信息

Department of Environmental Medicine and Public Health, Icahn School of Medicine at Mount Sinai, New York, NY, United States.

Channing Division of Network Medicine, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, United States; Department of Environmental Health, Harvard T.H. Chan School of Public Health, Boston, MA, United States.

出版信息

Environ Int. 2022 Jan;158:106957. doi: 10.1016/j.envint.2021.106957. Epub 2021 Oct 28.

Abstract

Exposure to traffic-related pollutants, including diesel exhaust, is associated with increased risk of cardiopulmonary disease and mortality; however, the precise biochemical pathways underlying these effects are not known. To investigate biological response mechanisms underlying exposure to traffic related pollutants, we used an integrated molecular response approach that included high-resolution metabolomic profiling and peripheral blood gene expression to identify biological responses to diesel exhaust exposure. Plasma samples were collected from 73 non-smoking males employed in the US trucking industry between February 2009 and October 2010, and analyzed using untargeted high-resolution metabolomics to characterize metabolite associations with shift- and week-averaged levels of elemental carbon (EC), organic carbon (OC) and particulate matter with diameter ≤ 2.5 μm (PM). Metabolic associations with EC, OC and PM were evaluated for biochemical processes known to be associated with disease risk. Annotated metabolites associated with exposure were then tested for relationships with the peripheral blood transcriptome using multivariate selection and network correlation. Week-averaged EC and OC levels, which were averaged across multiple shifts during the workweek, resulted in the greatest exposure-associated metabolic alterations compared to shift-averaged exposure levels. Metabolic changes associated with EC exposure suggest increased lipid peroxidation products, biomarkers of oxidative stress, thrombotic signaling lipids, and metabolites associated with endothelial dysfunction from altered nitric oxide metabolism, while OC exposures were associated with antioxidants, oxidative stress biomarkers and critical intermediates in nitric oxide production. Correlation with whole blood RNA gene expression provided additional evidence of changes in processes related to endothelial function, immune response, inflammation, and oxidative stress. We did not detect metabolic associations with PM. This study provides an integrated molecular assessment of human exposure to traffic-related air pollutants that includes diesel exhaust. Metabolite and transcriptomic changes associated with exposure to EC and OC are consistent with increased risk of cardiovascular diseases and the adverse health effects of traffic-related air pollution.

摘要

暴露于交通相关污染物,包括柴油废气,与心肺疾病和死亡率增加有关; 然而,这些影响的确切生化途径尚不清楚。为了研究交通相关污染物暴露的生物学反应机制,我们使用了一种综合的分子反应方法,包括高分辨率代谢组学分析和外周血基因表达,以确定对柴油废气暴露的生物学反应。从 2009 年 2 月至 2010 年 10 月期间在美国卡车运输行业工作的 73 名不吸烟男性中采集了血浆样本,并使用非靶向高分辨率代谢组学分析来分析特征代谢物与元素碳(EC)、有机碳(OC)和直径≤2.5μm 的颗粒物(PM)的班次和周平均水平的关联。评估了与疾病风险相关的已知生化过程的 EC、OC 和 PM 代谢关联。然后,使用多元选择和网络相关性测试与暴露相关的注释代谢物与外周血转录组之间的关系。与 EC 和 OC 暴露相关的代谢变化表明,与工作周内多个班次的平均暴露水平相比,周平均 EC 和 OC 水平导致了最大的暴露相关代谢改变。与 EC 暴露相关的代谢变化表明脂质过氧化产物增加,氧化应激标志物,血栓形成信号脂质,以及与一氧化氮代谢改变相关的内皮功能障碍代谢物,而 OC 暴露与抗氧化剂,氧化应激标志物和一氧化氮产生的关键中间产物相关。与全血 RNA 基因表达的相关性提供了与内皮功能、免疫反应、炎症和氧化应激相关过程变化的额外证据。我们没有检测到与 PM 相关的代谢关联。这项研究提供了对包括柴油废气在内的交通相关空气污染物的综合分子评估。与 EC 和 OC 暴露相关的代谢物和转录组变化与心血管疾病风险增加以及交通相关空气污染的不良健康影响一致。

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