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围生期低剂量 2,2',4,4'-四溴二苯醚暴露对大鼠仔代肝脏基因表达谱的影响

Global gene expression analysis in the livers of rat offspring perinatally exposed to low doses of 2,2',4,4'-tetrabromodiphenyl ether.

机构信息

Département Obstétrique Gynécologie, Faculté de Médecine et des Sciences de la Santé, Université de Sherbrooke, Québec, Canada.

出版信息

Environ Health Perspect. 2010 Jan;118(1):97-102. doi: 10.1289/ehp.0901031.

Abstract

BACKGROUND

Polybrominated diphenyl ethers are a group of flame-retardant chemicals appearing increasingly in the environment. Their health effects and mechanisms of toxicity are poorly understood.

OBJECTIVES

We screened for the sensitive effects and mechanisms of toxicity of 2,2 ,4,4 -tetra-bromodiphenyl ether (BDE-47) by analyzing the gene expression profile in rats exposed to doses comparable to human exposure.

METHODS

Wistar dams were exposed to vehicle or BDE-47 (0.002 and 0.2 mg/kg body weight) every fifth day from gestation day 15 to postnatal day 20 by injections to caudal vein. Total RNA was extracted from the livers of pups and hybridized to the whole-genome RNA expression micro-arrays. The list of genes 2-fold differentially expressed was exported to PANTHER and Ingenuity Systems for analysis of enriched ontology groups and molecular pathways.

RESULTS

Oxidoreductase and transferase protein families were enriched in exposed rats as were these biological process categories: carbohydrate metabolism; electron transport; and lipid, fatty acid, and steroid metabolism. Four signaling pathways (cascades of activation of drug-metabolizing enzymes) and 10 metabolic pathways were significantly enriched. Drug-metabolizing enzymes appear to be regulated by BDE-47 through an aryl hydrocarbon receptor-independent mechanism. Direct interaction with retinoid X receptor or its upstream cascade may be involved. The main metabolic effects consisted of activation of metabolic pathways: alpha- and omega-oxidation of fatty acids, glycolysis, and starch hydrolysis.

CONCLUSIONS

Altered expression of genes involved in metabolic and signaling pathways and functions of the organism occurs after perinatal exposure of rat offspring to BDE-47 at doses relevant for the general population.

摘要

背景

多溴联苯醚是一组阻燃化学物质,在环境中越来越常见。它们的健康影响和毒性机制还不太清楚。

目的

我们通过分析接触剂量与人类暴露相当的大鼠的基因表达谱,筛选出 2,2,4,4-四溴二苯醚(BDE-47)的敏感毒性效应和机制。

方法

妊娠第 15 天至出生后第 20 天,Wistar 孕鼠每隔 5 天通过尾静脉注射接受载体或 BDE-47(0.002 和 0.2 mg/kg 体重)。从幼崽的肝脏中提取总 RNA,并与全基因组 RNA 表达微阵列杂交。将表达倍数变化 2 倍的基因列表导出到 PANTHER 和 Ingenuity Systems,以分析丰富的本体组和分子途径。

结果

暴露组大鼠中氧化还原酶和转移酶蛋白家族以及这些生物过程类别富集:碳水化合物代谢;电子传递;以及脂质、脂肪酸和类固醇代谢。四个信号通路(药物代谢酶的激活级联)和 10 个代谢通路显著富集。BDE-47 似乎通过非芳香烃受体机制调节药物代谢酶。可能涉及与视黄醇 X 受体或其上游级联的直接相互作用。主要的代谢效应包括代谢途径的激活:脂肪酸的α-和ω-氧化、糖酵解和淀粉水解。

结论

在与一般人群相关的剂量下,BDE-47 对大鼠后代围产期暴露后,参与代谢和信号通路以及生物体功能的基因表达发生改变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6c40/2831975/3fc5c5257cf0/ehp-118-97f1.jpg

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