DNA methylation and gene expression changes in mouse mammary tissue during successive lactations: part I - the impact of inflammation.

IF 2.9 3区生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY

Epigenetics Pub Date : 2023-12-01 DOI:10.1080/15592294.2023.2215633

E Ivanova, C Hue-Beauvais, A Chaulot-Talmon, J Castille, J Laubier, C De Casanove, A Aubert-Frambourg, P Germon, H Jammes, F Le Provost

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引用次数: 1

Abstract

Mastitis is among the main reasons women cease breastfeeding, which leads to them supplementing breast milk with artificial formula. In farm animals, mastitis results in significant economic losses and the premature culling of some animals. Nevertheless, researchers do not know enough about the effect of inflammation on the mammary gland. This article discusses the changes to DNA methylation in mouse mammary tissue caused by lipopolysaccharide-induced inflammation (4 h post-injection of lipopolysaccharide). We analysed the expression of some genes related to mammary gland function, epigenetic regulation, and the immune response. The analysis focused on three comparisons: inflammation during the first lactation, inflammation during second lactation with no history of inflammation, and inflammation during second lactation with previous inflammation. We identified differentially methylated cytosines (DMCs), differentially methylated regions (DMRs), and some differentially expressed genes (DEGs) for each comparison. The three comparisons shared some DEGs; however, few DMCs and only one DMR were shared. These observations suggest that inflammation is one of several factors affecting epigenetic regulation during successive lactations. Furthermore, the comparison between animals in second lactation with and without inflammation, with no inflammation history during first lactation showed a different pattern compared to the other conditions in this experiment. This indicates that inflammation history plays an important role in determining epigenetic changes. The data presented in this study suggest that lactation rank and previous inflammation history are equally important when explaining mammary tissue gene expression and DNA methylation changes.Abbreviations: RRBS, reduced representation bisulfite sequencing; RT-qPCR, real-time quantitative polymerase chain reaction; MEC, mammary epithelial cells; TSS, transcription start site; TTS, transcription termination site; UTR, untranslated region; SINE, short interspersed nuclear element; LINE, long interspersed nuclear element; CGI, CpG island; DEG, differentially expressed gene; DMC, differentially methylated cytosine; DMR, differentially methylated region; GO term, gene ontology term; MF, molecular function; BP, biological process.

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连续哺乳期间小鼠乳腺组织DNA甲基化和基因表达变化:第一部分-炎症的影响。

乳房炎是女性停止母乳喂养的主要原因之一，这导致她们用人工配方奶粉补充母乳。在农场动物中，乳腺炎会导致巨大的经济损失和一些动物过早被扑杀。然而，研究人员对炎症对乳腺的影响知之甚少。本文讨论了脂多糖诱导的炎症（注射脂多糖后4小时）引起的小鼠乳腺组织DNA甲基化的变化。我们分析了一些与乳腺功能、表观遗传学调控和免疫反应相关的基因的表达。分析集中在三个比较上：第一次哺乳期间的炎症，第二次哺乳期间没有炎症史的炎症，以及第二次泌乳期间有既往炎症的炎症。我们在每次比较中鉴定了差异甲基化胞嘧啶（DMCs）、差异甲基化区域（DMRs）和一些差异表达基因（DEG）。三次比较共有一些DEG；然而，共享的DMC很少，只有一个DMR。这些观察结果表明，炎症是影响连续哺乳期表观遗传学调控的几个因素之一。此外，与本实验中的其他条件相比，第二次哺乳期有和没有炎症、第一次哺乳期没有炎症史的动物之间的比较显示出不同的模式。这表明炎症史在决定表观遗传学变化中起着重要作用。本研究中提供的数据表明，在解释乳腺组织基因表达和DNA甲基化变化时，泌乳级别和既往炎症史同样重要。缩写：RRBS，还原表示亚硫酸氢盐测序；RT-qPCR，实时定量聚合酶链式反应；乳腺上皮细胞；TSS，转录起始位点；TTS，转录终止位点；UTR，非翻译区；SINE，短穿插核元素；LINE，长穿插的核元素；CGI，CpG岛；DEG，差异表达基因；DMC，差异甲基化胞嘧啶；DMR，差异甲基化区域；GO术语、基因本体论术语；MF，分子功能；BP，生物过程。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Epigenetics 生物-生化与分子生物学

CiteScore

6.80

自引率

2.70%

发文量

审稿时长

3-8 weeks

期刊介绍： Epigenetics publishes peer-reviewed original research and review articles that provide an unprecedented forum where epigenetic mechanisms and their role in diverse biological processes can be revealed, shared, and discussed. Epigenetics research studies heritable changes in gene expression caused by mechanisms others than the modification of the DNA sequence. Epigenetics therefore plays critical roles in a variety of biological systems, diseases, and disciplines. Topics of interest include (but are not limited to): DNA methylation Nucleosome positioning and modification Gene silencing Imprinting Nuclear reprogramming Chromatin remodeling Non-coding RNA Non-histone chromosomal elements Dosage compensation Nuclear organization Epigenetic therapy and diagnostics Nutrition and environmental epigenetics Cancer epigenetics Neuroepigenetics