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Late gestational intermittent hypoxia induces metabolic and epigenetic changes in male adult offspring mice

机译:晚期妊娠间歇性缺氧诱导男性成人后代小鼠的代谢和表观遗传变化

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摘要

Pregnancy, particularly late gestation (LG), has been associated with a relatively high prevalence of obstructive sleep apnoea (OSA). Intermittent hypoxia (IH), a hallmark of OSA, could impose significant long-term effects on somatic growth, energy homeostasis, and metabolic function in offspring. We hypothesized that IH during late pregnancy (LG-IH) may increase the propensity for metabolic dysregulation and obesity in adult offspring via epigenetic modifications. Time-pregnant female C57BL/6 mice were exposed to LG-IH or room air (LG-RA) during days 13-18 of gestation. At 24 weeks, blood samples were collected from offspring mice for lipid profiles and insulin resistance, indirect calorimetry was performed and visceral white adipose tissues (VWAT) were assessed for inflammatory cells as well as for differentially methylated gene regions (DMRs) using a methylated DNA immunoprecipitation on chip (MeDIP-chip). Body weight, food intake, adiposity index, fasting insulin, triglycerides and cholesterol levels were all significantly higher in LG-IH male but not female offspring. LG-IH also altered metabolic expenditure and locomotor activities in male offspring, and increased number of pro-inflammatory macrophages emerged in VWAT along with 1520DMRs (P < 0.0001), associated with 693 genes. Pathway analyses showed that genes affected by LG-IH were mainly associated with molecular processes related to metabolic regulation and inflammation. LG-IH induces metabolic dysfunction as reflected by increased body weight and adiposity index in adult male offspring that is paralleled by epigenomic alterations and inflammation in VWAT. Thus, perturbations to fetal environment by OSA during pregnancy can have long-term detrimental effects on the fetus, and lead to persistent metabolic dysfunction in adulthood.
机译:怀孕,特别晚期妊娠(LG),与阻塞性睡眠呼吸暂停(OSA)的相对较高的患病率有关。间歇性缺氧(IH),OSA的标志,可能对体细胞生长,能量稳态和后代代谢功能施加显着的长期影响。我们假设妊娠晚期(LG-IH)的IH可以通过表观遗传修饰增加成人后代代谢失调和肥胖的倾向。在妊娠期的第13-18天期间暴露于Lg-1H或室内空气(LG-RA)的时间孕妇C57BL / 6小鼠。在24周时,从后代小鼠收集血液样品,用于脂质谱,进行间接量热法,对炎性细胞以及使用甲基化DNA的差异甲基化基因区(DMR)评估内脏白色脂肪组织(VWAT)芯片上的免疫沉淀(Medip-Chip)。体重,食物摄入,肥胖指数,禁食胰岛素,甘油三酯和胆固醇水平在LG-IH雄性中显着高,但不是女性后代。 LG-IH还改变了男性后代的代谢支出和运动活动,并且vwat中出现的促炎巨噬细胞的数量增加以及1520dmrs(p <0.0001),与693基因相关。途径分析表明,受LG-IH影响的基因主要与与代谢调节和炎症有关的分子过程有关。 LG-IH诱导代谢功能障碍,如成年男性后代的体重增加和肥胖指数的反射,该雄性后代在vwat中的表观元素改变和炎症平行。因此,怀孕期间OSA对胎儿环境的扰动可对胎儿产生长期不利影响,并导致成年期持续的代谢功能障碍。

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  • 来源
    《The Journal of Physiology》 |2017年第8期|共18页
  • 作者单位

    Univ Chicago Sect Pediat Sleep Med Dept Pediat Room 4100 900 E 57th St Mailbox 4 Chicago IL;

    Univ Chicago Sect Pediat Sleep Med Dept Pediat Room 4100 900 E 57th St Mailbox 4 Chicago IL;

    Univ Chicago Sect Pediat Sleep Med Dept Pediat Room 4100 900 E 57th St Mailbox 4 Chicago IL;

    Univ Chicago Sect Endocrinol &

    Metab Dept Med Room 4100 900 E 57th St Mailbox 4 Chicago IL;

    Univ Chicago Pritzker Sch Med Div Biol Sci Ctr Res Informat Room 4100 900 E 57th St Mailbox 4;

    Univ Chicago Pritzker Sch Med Div Biol Sci Ctr Res Informat Room 4100 900 E 57th St Mailbox 4;

    Univ Chicago Sect Pediat Sleep Med Dept Pediat Room 4100 900 E 57th St Mailbox 4 Chicago IL;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 人体生理学;
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