暴露于钼酸盐会导致代谢紊乱:小鼠尿液元素组和血清代谢组的综合研究。

Toxics Pub Date : 2024-04-14 DOI:10.3390/toxics12040288
Kun Zhou, Miaomiao Tang, Wei Zhang, Yanling Chen, Yusheng Guan, Rui Huang, Jiawei Duan, Zibo Liu, Xiaoming Ji, Yingtong Jiang, Yanhui Hu, Xiaoling Zhang, Jingjing Zhou, Minjian Chen
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引用次数: 0

摘要

钼酸盐的使用日益增多,引起了人们对其对人体潜在毒性的关注。然而,在目前的人体接触水平下,钼酸盐的潜在毒性在很大程度上仍是未知数。人类因暴露于环境污染物而引起的内源性代谢改变与许多疾病的发生和发展有关。本研究将八周大的雄性 C57 小鼠暴露于与人类相关剂量(0.01 和 1 毫克/千克/天)的钼酸钠,为期八周。电感耦合等离子体质谱法(ICP-MS)和超高效液相色谱串联质谱法(UPLC-MS)分别用于评估小鼠尿液中元素水平和血清代谢物的变化。我们的研究还纳入了 NHANES 2017-2018 年人口数据库中的 838 名受试者,以验证在小鼠体内发现的钼与镉之间的关联。对小鼠代谢组的分析表明,血清中的四种代谢物出现了显著变化,包括5-氨基乙酰丙酸、乙醇酸、l-乙酰肉碱和2,3-二羟基丙基辛酸酯。元素组分析表明,接触钼酸盐后,小鼠尿液中的镉含量明显增加。值得注意的是,NHANES 数据库中的人体钼含量也与镉含量呈正相关。进一步分析发现,小鼠体内的镉与辛酸 2,3-二羟基丙酯呈正相关。总之,这些研究结果表明,钼酸盐暴露会扰乱氨基酸和脂质代谢,而钼酸盐改变的镉水平可能是扰乱氨基酸和脂质代谢的部分原因。元素组和代谢组数据的整合提供了有关钼酸盐诱导的代谢紊乱以及与人类暴露水平相关的毒性的敏感信息。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Exposure to Molybdate Results in Metabolic Disorder: An Integrated Study of the Urine Elementome and Serum Metabolome in Mice.
The increasing use of molybdate has raised concerns about its potential toxicity in humans. However, the potential toxicity of molybdate under the current level of human exposure remains largely unknown. Endogenous metabolic alterations that are caused in humans by environmental exposure to pollutants are associated with the occurrence and progression of many diseases. This study exposed eight-week-old male C57 mice to sodium molybdate at doses relevant to humans (0.01 and 1 mg/kg/day) for eight weeks. Inductively coupled plasma mass spectrometry (ICP-MS) and ultra-performance liquid chromatography tandem mass spectrometry (UPLC-MS) were utilized to assess changes in urine element levels and serum metabolites in mice, respectively. A total of 838 subjects from the NHANES 2017-2018 population database were also included in our study to verify the associations between molybdenum and cadmium found in mice. Analysis of the metabolome in mice revealed that four metabolites in blood serum exhibited significant changes, including 5-aminolevulinic acid, glycolic acid, l-acetylcarnitine, and 2,3-dihydroxypropyl octanoate. Analysis of the elementome revealed a significant increase in urine levels of cadmium after molybdate exposure in mice. Notably, molybdenum also showed a positive correlation with cadmium in humans from the NHANES database. Further analysis identified a positive correlation between cadmium and 2,3-dihydroxypropyl octanoate in mice. In conclusion, these findings suggest that molybdate exposure disrupted amino acid and lipid metabolism, which may be partially mediated by molybdate-altered cadmium levels. The integration of elementome and metabolome data provides sensitive information on molybdate-induced metabolic disorders and associated toxicities at levels relevant to human exposure.
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