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斑马鱼在发育过程中暴露于邻苯二甲酸二(2-乙基己基)酯和5-氮杂胞苷后,保守非基因元件处的DNA甲基化差异及跨代遗传证据。

Differential DNA methylation at conserved non-genic elements and evidence for transgenerational inheritance following developmental exposure to mono(2-ethylhexyl) phthalate and 5-azacytidine in zebrafish.

作者信息

Kamstra Jorke H, Sales Liana Bastos, Aleström Peter, Legler Juliette

机构信息

Faculty of Veterinary Medicine, Department of Basic Sciences and Aquatic Medicine, CoE CERAD, Norwegian University of Life Sciences, P.O. Box 8146 Dep., 0033 Oslo, Norway.

Institute for Environmental Studies, VU University Amsterdam, Amsterdam, The Netherlands.

出版信息

Epigenetics Chromatin. 2017 Apr 12;10:20. doi: 10.1186/s13072-017-0126-4. eCollection 2017.

Abstract

BACKGROUND

Exposure to environmental stressors during development may lead to latent and transgenerational adverse health effects. To understand the role of DNA methylation in these effects, we used zebrafish as a vertebrate model to investigate heritable changes in DNA methylation following chemical-induced stress during early development. We exposed zebrafish embryos to non-embryotoxic concentrations of the biologically active phthalate metabolite mono(2-ethylhexyl) phthalate (MEHP, 30 µM) and the DNA methyltransferase 1 inhibitor 5-azacytidine (5AC, 10 µM). Direct, latent and transgenerational effects on DNA methylation were assessed using global, genome-wide and locus-specific DNA methylation analyses.

RESULTS

Following direct exposure in zebrafish embryos from 0 to 6 days post-fertilization, genome-wide analysis revealed a multitude of differentially methylated regions, strongly enriched at conserved non-genic elements for both compounds. Pathways involved in adipogenesis were enriched with the putative obesogenic compound MEHP. Exposure to 5AC resulted in enrichment of pathways involved in embryonic development and transgenerational effects on larval body length. Locus-specific methylation analysis of 10 differentially methylated sites revealed six of these loci differentially methylated in sperm sampled from adult zebrafish exposed during development to 5AC, and in first and second generation larvae. With MEHP, consistent changes were found at 2 specific loci in first and second generation larvae.

CONCLUSIONS

Our results suggest a functional role for DNA methylation on cis-regulatory conserved elements following developmental exposure to compounds. Effects on these regions are potentially transferred to subsequent generations.

摘要

背景

发育过程中暴露于环境应激源可能导致潜在的和跨代的不良健康影响。为了解DNA甲基化在这些影响中的作用,我们使用斑马鱼作为脊椎动物模型,研究早期发育过程中化学诱导应激后DNA甲基化的遗传变化。我们将斑马鱼胚胎暴露于生物活性邻苯二甲酸酯代谢物单(2-乙基己基)邻苯二甲酸酯(MEHP,30µM)和DNA甲基转移酶1抑制剂5-氮杂胞苷(5AC,10µM)的非胚胎毒性浓度下。使用全局、全基因组和位点特异性DNA甲基化分析评估对DNA甲基化的直接、潜在和跨代影响。

结果

在受精后0至6天对斑马鱼胚胎进行直接暴露后,全基因组分析揭示了大量差异甲基化区域,两种化合物在保守的非基因元件中均强烈富集。参与脂肪生成的途径富含假定的致肥胖化合物MEHP。暴露于5AC导致参与胚胎发育的途径富集以及对幼虫体长的跨代影响。对10个差异甲基化位点的位点特异性甲基化分析显示,在发育过程中暴露于5AC的成年斑马鱼的精子以及第一代和第二代幼虫中,这些位点中有6个差异甲基化。对于MEHP,在第一代和第二代幼虫的2个特定位点发现了一致的变化。

结论

我们的结果表明,发育过程中暴露于化合物后,DNA甲基化在顺式调控保守元件上具有功能作用。对这些区域的影响可能会传递给后代。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3076/5389146/d8c4f25b9d9e/13072_2017_126_Fig1_HTML.jpg

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