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大鼠亚慢性暴露后,二元和三元混合物中苯、三氯乙烯和甲基汞对肝脏和肾脏交互作用的转录组学分析。

Transcriptomics analysis of interactive effects of benzene, trichloroethylene and methyl mercury within binary and ternary mixtures on the liver and kidney following subchronic exposure in the rat.

作者信息

Hendriksen Peter J M, Freidig Andreas P, Jonker Diana, Thissen Uwe, Bogaards Jan J P, Mumtaz Moiz M, Groten John P, Stierum Rob H

机构信息

TNO Quality of Life, Zeist, The Netherlands.

出版信息

Toxicol Appl Pharmacol. 2007 Dec 1;225(2):171-88. doi: 10.1016/j.taap.2007.08.017. Epub 2007 Aug 29.

Abstract

The present research aimed to study the interaction of three chemicals, methyl mercury, benzene and trichloroethylene, on mRNA expression alterations in rat liver and kidney measured by microarray analysis. These compounds were selected based on presumed different modes of action. The chemicals were administered daily for 14 days at the Lowest-Observed-Adverse-Effect-Level (LOAEL) or at a two- or threefold lower concentration individually or in binary or ternary mixtures. The compounds had strong antagonistic effects on each other's gene expression changes, which included several genes encoding Phase I and II metabolizing enzymes. On the other hand, the mixtures affected the expression of "novel" genes that were not or little affected by the individual compounds. The three compounds exhibited a synergistic interaction on gene expression changes at the LOAEL in the liver and both at the sub-LOAEL and LOAEL in the kidney. Many of the genes induced by mixtures but not by single compounds, such as Id2, Nr2f6, Tnfrsf1a, Ccng1, Mdm2 and Nfkb1 in the liver, are known to affect cellular proliferation, apoptosis and tissue-specific function. This indicates a shift from compound specific response on exposure to individual compounds to a more generic stress response to mixtures. Most of the effects on cell viability as concluded from transcriptomics were not detected by classical toxicological endpoints illustrating the benefit of increased sensitivity of assessing gene expression profiling. These results emphasize the benefit of applying toxicogenomics in mixture interaction studies, which yields biomarkers for joint toxicity and eventually can result in an interaction model for most known toxicants.

摘要

本研究旨在通过微阵列分析研究三种化学物质——甲基汞、苯和三氯乙烯对大鼠肝脏和肾脏中mRNA表达变化的相互作用。这些化合物是根据假定的不同作用模式选择的。这些化学物质分别或以二元或三元混合物的形式,以最低观察到有害效应水平(LOAEL)或低两到三倍的浓度每日给药14天。这些化合物对彼此的基因表达变化具有强烈的拮抗作用,其中包括几个编码I相和II相代谢酶的基因。另一方面,混合物影响了“新”基因的表达,这些基因未受或仅受单个化合物的轻微影响。这三种化合物在肝脏的LOAEL水平以及在肾脏的低于LOAEL和LOAEL水平上,对基因表达变化表现出协同相互作用。许多由混合物而非单一化合物诱导的基因,如肝脏中的Id2、Nr2f6、Tnfrsf1a、Ccng1、Mdm2和Nfkb1,已知会影响细胞增殖、凋亡和组织特异性功能。这表明从暴露于单个化合物时的化合物特异性反应转变为对混合物更普遍的应激反应。转录组学得出的对细胞活力的大多数影响,经典毒理学终点未检测到,这说明了评估基因表达谱灵敏度提高的益处。这些结果强调了在混合物相互作用研究中应用毒理基因组学的益处,它能产生联合毒性的生物标志物,并最终可形成一个针对大多数已知毒物的相互作用模型。

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