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

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

Key points Late gestation during pregnancy has been associated with a relatively high prevalence of obstructive sleep apnoea (OSA). Intermittent hypoxia, a hallmark of OSA, could impose significant long‐term effects on somatic growth, energy homeostasis and metabolic function in offspring. Here we s...

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Veröffentlicht in:The Journal of physiology 2017-04, Vol.595 (8), p.2551-2568
Hauptverfasser: Khalyfa, Abdelnaby, Cortese, Rene, Qiao, Zhuanhong, Ye, Honggang, Bao, Riyue, Andrade, Jorge, Gozal, David
Format: Artikel
Sprache:eng
Schlagworte:
Adipose Tissue - metabolism
Animals
Epigenesis, Genetic - physiology
epigenetics
Female
Gene Regulatory Networks - physiology
gestation
Hypoxia
Hypoxia - complications
Hypoxia - genetics
Hypoxia - metabolism
Insulin Resistance - physiology
intermittent hypoxia
Male
Maternal, Fetal and Neonatal Physiology
Metabolic Diseases - etiology
Metabolic Diseases - genetics
Metabolic Diseases - metabolism
metabolic syndrome
methylation
Mice
Mice, Inbred C57BL
Pregnancy
Pregnancy Complications - genetics
Pregnancy Complications - metabolism
Prenatal Exposure Delayed Effects - etiology
Prenatal Exposure Delayed Effects - genetics
Prenatal Exposure Delayed Effects - metabolism
Research Paper
Respiratory
Respiratory Physiology
sleep apnea
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Zusammenfassung:Key points Late gestation during pregnancy has been associated with a relatively high prevalence of obstructive sleep apnoea (OSA). Intermittent hypoxia, a hallmark of OSA, could impose significant long‐term effects on somatic growth, energy homeostasis and metabolic function in offspring. Here we show that late gestation intermittent hypoxia 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 visceral white adipose tissue. Fetal perturbations by OSA during pregnancy impose long‐term detrimental effects manifesting as metabolic dysfunction in adult male offspring. 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 1520 DMRs (P 
ISSN:0022-3751
1469-7793
DOI:10.1113/JP273570