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Obesogen effect of bisphenol S alters mRNA expression and DNA methylation profiling in male mouse liver

机译:双酚S改变雄性小鼠肝脏的mRNA表达和DNA甲基化分析的血吸虫效应

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摘要

Environmental pollution is increasingly considered an important factor involved in the obesity incidence. Endocrine disruptors (EDs) are important actors in the concept of DOHaD (Developmental Origins of Health and Disease), where epigenetic mechanisms play crucial roles. Bisphenol A (BPA), a monomer used in the manufacture of plastics and resins is one of the most studied obesogenic endocrine disruptor. Bisphenol S (BPS), a BPA substitute, has the same obesogenic properties, acting at low doses with a sexspecific effect following perinatal exposure. Since the liver is a major organ in regulating body lipid homeostasis, we investigated gene expression and DNA methylation under low-dose BPS exposure. The BPS obesogenic effect was associated with an increase of hepatic triglyceride content. These physiological disturbances were accompanied by genome-wide changes in gene expression (1366 genes significantly modified more than 1.5 -fold).Gene ontology analysis revealed alteration of gene cascades involved in protein translation and complement regulation. It was associated with hepatic DNA hypomethylation in autosomes and hypermethylation in sex chromosomes. Although no systematic correlation has been found between gene repression and hypermethylation, several genes related to liver metabolism were either hypermethylated (Acsl4, Gpr40, Cel, Ppar delta, Abca6, Ces3a, Sgms2) or hypomethylated (Sogal, Gpihbpl, Nr1d2, Mlxipl, Rps6kb2, Esrrb, Thra, Cidec). In specific cases (Hapin4, ApoA4, Cidec, genes involved in lipid metabolism and liver fibrosis) mRNA upregulation was associated with hypomethylation. In conclusion, we show for the first time wide disruptive physiological effects of low-dose of BPS, which raises the question of its harmlessness as an industrial substitute for BPA. (C) 2019 Elsevier Ltd. All rights reserved.
机译:环境污染越来越多地被认为是肥胖发病率的重要因素。内分泌干​​扰者(EDS)是杜哈德(健康和疾病发育起源)概念中的重要作用者,其中表观遗传机制起到关键的作用。双酚A(BPA),一种用于制造塑料和树脂的单体是最受研究的嗜噬内分泌破坏器之一。双酚S(BPS)是BPA替代品具有相同的富含噬菌性,在低剂量下作用,围产产暴露后的性别特异性。由于肝脏是调节身体血脂性稳态的主要器官,因此我们在低剂量BPS暴露下调查基因表达和DNA甲基化。 BPS贫化效果与肝甘油三酯含量的增加有关。这些生理障碍伴随着基因表达的全基因组变化(1366个基因显着修饰超过1.5多元)。否本体论分析显示蛋白质翻译和补体调节中的基因级联的改变。它与肝脏DNA低甲基化与性染色体中的高甲基化有关。尽管基因抑制和高甲基化之间没有发现系统相关性,但是与肝脏代谢有关的几种基因是高甲基化(ACSL4,GPR40,CEL,PPARδ,ABCA6,CES3A,SGMS2或甲基化(SOGAL,GPIHBPL,NR1D2,MLXIPL,RPS6KB2 ,ESRRB,THRA,CIDEC)。在具体情况下(Hapin4,ApoA4,CIDEC,参与脂质代谢和肝纤维化的基因)mRNA上调与低甲基化有关。总之,我们展示了低剂量BPS的宽大破坏性生理作用,这提出了其对BPA工业替代品的无害的问题。 (c)2019 Elsevier Ltd.保留所有权利。

著录项

  • 来源
    《Chemosphere》 |2020年第2期|125092.1-125092.14|共14页
  • 作者单位

    Univ Bourgogne Franche Comte UMR1231 LNC F-21000 Dijon France|AgroSup UMR1231 LNC F-21000 Dijon France|INSERM UMR1231 Nutr Physiol & Toxicol Team NUTox LNC F-21000 Dijon France;

    Inst Cochin U1016 INSERM FGTB F-75014 Paris France|CNRS UMR8104 F-75014 Paris France|Univ Sorbonne Paris Cite F-75014 Paris France;

    Univ Bourgogne Franche Comte UMR1231 LNC F-21000 Dijon France|AgroSup UMR1231 LNC F-21000 Dijon France|INSERM UMR1231 Nutr Physiol & Toxicol Team NUTox LNC F-21000 Dijon France;

    Univ Bourgogne Franche Comte UMR1231 LNC F-21000 Dijon France|AgroSup UMR1231 LNC F-21000 Dijon France|INSERM UMR1231 Nutr Physiol & Toxicol Team NUTox LNC F-21000 Dijon France;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Bisphenol S; Obesogen; Perinatal chronic exposure; Liver; DNA methylation; Transcriptome;

    机译:双酚S;obesogen;围产期慢性暴露;肝脏;DNA甲基化;转录组;

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