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>Reprogramming of miR-181a/DNA methylation patterns contribute to the maternal nicotine exposure-induced fetal programming of cardiac ischemia-sensitive phenotype in postnatal life
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Reprogramming of miR-181a/DNA methylation patterns contribute to the maternal nicotine exposure-induced fetal programming of cardiac ischemia-sensitive phenotype in postnatal life
Background: E-cigarette and other novel electronic nicotine delivery systems (ENDS) have recently entered the market at a rapid pace. The community desperately needs answers about the health effects of ENDS. The present study tested the hypothesis that perinatal nicotine exposure (PNE) causes a gender-dependent increase in vulnerability of the heart to ischemia-reperfusion (I/R) injury and cardiac dysfunction in male rat offspring via reprogramming of the miRNA-181a (miR-181a)-mediated signaling pathway and that miR-181a antisense could rescue this phenotype. Methods: Nicotine or saline was administered to pregnant rats via subcutaneous osmotic minipumps from gestational day 4 until postnatal day 10. Cardiac function and molecular biological experiments were conducted in ~3- month-old offspring. Results: PNE enhanced I/R-induced cardiac dysfunction and infarction in adult male but not in female offspring, which was associated with miR-181a over-expression in left ventricle tissues. In addition, PNE enhanced offspring cardiac angiotensin receptor (ATR) expressions via specific CpG hypomethylation of AT 1 R/AT 2 R promoter. Furthermore, PNE attenuated cardiac lncRNA H19 levels, but up-regulated cardiac TGF-β/Smads family proteins and consequently up-regulated autophagy-related protein (Atg-5, beclin-1, LC3 II, p62) expression in the male offspring. Of importance, treatment with miR-181a antisense eliminated the PNE's effect on miR-181a expression/H19 levels and reversed PNE-mediated I/R-induced cardiac infarction and dysfunction in male offspring. Furthermore, miR-181a antisense also attenuated the effect of PNE on AT 1 R/AT 2 R/TGF-β/Smads/autophagy-related biomarkers in the male offspring. Conclusion: Our data suggest that PNE could induce a reprogramming of cardiac miR-181a expression/DNA methylation pattern, which epigenetically modulates ATR/TGF-β/autophagy signaling pathways, leading to gender-dependent development of ischemia-sensitive phenotype in postnatal life. Furthermore, miR-181a could severe as a potential therapeutic target for rescuing this phenotype.? The author(s).
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机译:背景:电子烟和其他新型电子尼古丁交付系统(终端)最近进入了快速的市场。社区拼命地需要答案关于结束的健康影响。本研究检测了围产尼古丁暴露(PNE)的假设,导致心脏脆性的性别依赖性增加,通过重新编程MiRNA-181A(MIR)对雄性大鼠后代的缺血再灌注(I / R)损伤和心脏功能障碍(MIR -181a)介导的信号通路,MiR-181a反义可以拯救这种表型。方法:通过从妊娠第4天的皮下渗透微型铝施用尼古丁或盐水到孕腺大鼠直至产后第10天。在〜3个月的后代进行心功能和分子生物实验。结果:PNE增强I / R诱导的心脏功能障碍和成年男性的梗塞,但不在雌性后代,其与左心室组织中的miR-181a过表达有关。此外,PNE通过特异性CpG低甲基化在1 r / ut启动子的特异性Cpg甲基化,PNE增强了后代心血管素受体(ATR)表达。此外,PNE减弱心脏LNCRNA H19水平,但上调的心脏TGF-β/ Smads系列蛋白质,并因此在雄性后代中的上调的自噬相关蛋白(ATG-5,BEC11,LC3 II,P62)表达。重要性,用miR-181a反义的治疗消除了对miR-181a表达/ h19水平的pne的影响,并逆转Pne介导的I / R诱导的心脏梗死和雄性后代的功能障碍。此外,的miR-181A的反义也衰减PNE的效果上AT 1个R / AT 2 R / TGF-β/ Smad蛋白/自噬相关生物标志物在雄性后代。结论:我们的数据表明,PNE可以诱导心脏miR-181A表达/ DNA甲基化模式的重新编程,其表现出ATR / TGF-β/自噬信号传导途径,导致出生后生命中缺血敏感表型的性别依赖性发展。此外,miR-181a可以严重作为抵抗这种表型的潜在治疗靶标。作者。
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