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尿液中的挥发性有机化合物(VOC)代谢物与全身炎症水平升高有关,吸烟者被确定为易感人群。

Volatile organic compounds (VOC) metabolites in urine are associated with increased systemic inflammation levels, and smokers are identified as a vulnerable population.

作者信息

Hu Yuanzhuo, Niu Zhiping, Cao Changsheng, Gao Jun, Pan Miaoting, Cai Yunfei, Zhao Zhuohui

机构信息

Department of Environmental Health, School of Public Health, NHC Key Laboratory of Health Technology Assessment (Fudan University), Key Laboratory of Public Health Safety of the Ministry of Education, Fudan University, Shanghai 200032, China.

Institute of HVAC Engineering, School of Mechanical Engineering, Tongji University, Shanghai 200092, China.

出版信息

Ecotoxicol Environ Saf. 2024 Dec;288:117398. doi: 10.1016/j.ecoenv.2024.117398. Epub 2024 Nov 29.

Abstract

BACKGROUND

Previous studies indicated that exposure to VOCs was linked to increased systemic inflammation levels. However, the dose-response relationships between urine VOCs metabolites and systemic inflammation have not been established, and the key metabolite of the toxic compounds has not been identified.

METHODS

We used data in 7007 US adults in the NHANES cycles (2011-2018) across 8 years. Urinary VOC metabolites were measured using ultra-performance liquid chromatography and electrospray tandem mass spectrometry (UPLC-ESI/MSMS). VOC metabolites were adjusted by urinary creatinine level before analysis. Systemic inflammation was assessed by systemic immune-inflammation index (SII) and systemic inflammation response index (SIRI) indices. Generalized linear models, restricted cubic splines (RCS), and weighted quantile sum (WQS) regression were applied to evaluate the associations, exposure-response (E-R) curve and identify the key contributor compound, adjusting for gender, age, race, BMI, marital condition, education level, smoking level, alcohol consumption and physical activity. Smoking status was assessed as an effect modifier.

RESULTS

Significant and robust positive correlations were found between 8 VOC metabolites and both SII and SIRI. They were N-Acetyl-S-(2-carboxyethyl)-L-cysteine (CEMA), N-Acetyl-S-(2-cyanoethyl)-L-cysteine (CYMA), N-Acetyl-S-(3,4-dihydroxybutyl)-L-cysteine (DHBMA), N-Acetyl-S-(3-hydroxypropyl)-L-cysteine (3HPMA), mandelic acid (MA), N-Acetyl-S-(4-hydroxy-2-butenyl)-L-cysteine (MHBMA3), phenylglyoxylic acid (PGA), and N-Acetyl-S-(3-hydroxypropyl-1-methyl)-L-cysteine (HPMMA). The RCS curves showed J-shaped or exponential shaped E-R relationships for most VOC metabolites. WQS regression found that exposure to the mixture of VOC metabolites was related to increased systemic inflammation, and MA was the key VOC metabolite contributing most to systemic inflammation levels. Smokers exhibited higher levels of urinary VOCs and larger susceptibility to VOC-related increases in SII and SIRI compared to non-smokers.

CONCLUSION

This study demonstrated a strong link between urinary VOC metabolites and increased systemic inflammation, and smokers were more susceptible. Our findings highlighted the significance of reducing VOC exposure to mitigate the inflammation levels, particularly for smokers.

摘要

背景

先前的研究表明,接触挥发性有机化合物(VOCs)与全身炎症水平升高有关。然而,尿液中VOCs代谢物与全身炎症之间的剂量反应关系尚未确立,且有毒化合物的关键代谢物也未被识别。

方法

我们使用了美国国家健康与营养检查调查(NHANES)2011 - 2018年8个周期中7007名美国成年人的数据。使用超高效液相色谱和电喷雾串联质谱法(UPLC - ESI/MSMS)测量尿液中的VOC代谢物。在分析前,VOC代谢物通过尿肌酐水平进行校正。通过全身免疫炎症指数(SII)和全身炎症反应指数(SIRI)评估全身炎症。应用广义线性模型、受限立方样条(RCS)和加权分位数和(WQS)回归来评估关联、暴露反应(E - R)曲线,并识别关键贡献化合物,同时对性别、年龄、种族、体重指数、婚姻状况、教育水平、吸烟程度、饮酒量和身体活动进行校正。吸烟状况被评估为效应修饰因子。

结果

发现8种VOC代谢物与SII和SIRI之间存在显著且稳健的正相关。它们分别是N - 乙酰 - S -(2 - 羧乙基)- L - 半胱氨酸(CEMA)、N - 乙酰 - S -(2 - 氰乙基)- L - 半胱氨酸(CYMA)、N - 乙酰 - S -(3,4 - 二羟基丁基)- L - 半胱氨酸(DHBMA)、N - 乙酰 - S -(3 - 羟丙基)- L - 半胱氨酸(3HPMA)、扁桃酸(MA)、N - 乙酰 - S -(4 - 羟基 - 2 - 丁烯基)- L - 半胱氨酸(MHBMA3)、苯甲酰甲酸(PGA)和N - 乙酰 - S -(3 - 羟丙基 - 1 - 甲基)- L - 半胱氨酸(HPMMA)。RCS曲线显示大多数VOC代谢物呈J形或指数形的E - R关系。WQS回归发现,接触VOC代谢物混合物与全身炎症增加有关,且MA是对全身炎症水平贡献最大的关键VOC代谢物。与非吸烟者相比,吸烟者尿液中VOCs水平更高,对VOC相关的SII和SIRI升高更敏感。

结论

本研究证明尿液中VOC代谢物与全身炎症增加之间存在紧密联系,且吸烟者更易受影响。我们的研究结果突出了减少VOC暴露以减轻炎症水平的重要性,尤其是对吸烟者而言。

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