Division of Exercise Physiology, West Virginia University School of Medicine, PO Box 9227, 1 Medical Center Drive, Morgantown, WV, 26506, USA.
Mitochondria, Metabolism & Bioenergetics Working Group, West Virginia University School of Medicine, Morgantown, WV, USA.
Part Fibre Toxicol. 2019 Jun 18;16(1):24. doi: 10.1186/s12989-019-0310-8.
Nano-titanium dioxide (nano-TiO) is amongst the most widely utilized engineered nanomaterials (ENMs). However, little is known regarding the consequences maternal ENM inhalation exposure has on growing progeny during gestation. ENM inhalation exposure has been reported to decrease mitochondrial bioenergetics and cardiac function, though the mechanisms responsible are poorly understood. Reactive oxygen species (ROS) are increased as a result of ENM inhalation exposure, but it is unclear whether they impact fetal reprogramming. The purpose of this study was to determine whether maternal ENM inhalation exposure influences progeny cardiac development and epigenomic remodeling.
Pregnant FVB dams were exposed to nano-TiO aerosols with a mass concentration of 12.09 ± 0.26 mg/m starting at gestational day five (GD 5), for 6 h over 6 non-consecutive days. Aerosol size distribution measurements indicated an aerodynamic count median diameter (CMD) of 156 nm with a geometric standard deviation (GSD) of 1.70. Echocardiographic imaging was used to assess cardiac function in maternal, fetal (GD 15), and young adult (11 weeks) animals. Electron transport chain (ETC) complex activities, mitochondrial size, complexity, and respiration were evaluated, along with 5-methylcytosine, Dnmt1 protein expression, and Hif1α activity. Cardiac functional analyses revealed a 43% increase in left ventricular mass and 25% decrease in cardiac output (fetal), with an 18% decrease in fractional shortening (young adult). In fetal pups, hydrogen peroxide (HO) levels were significantly increased (~ 10 fold) with a subsequent decrease in expression of the antioxidant enzyme, phospholipid hydroperoxide glutathione peroxidase (GPx4). ETC complex activity IV was decreased by 68 and 46% in fetal and young adult cardiac mitochondria, respectively. DNA methylation was significantly increased in fetal pups following exposure, along with increased Hif1α activity and Dnmt1 protein expression. Mitochondrial ultrastructure, including increased size, was observed at both fetal and young adult stages following maternal exposure.
Maternal inhalation exposure to nano-TiO results in adverse effects on cardiac function that are associated with increased HO levels and dysregulation of the Hif1α/Dnmt1 regulatory axis in fetal offspring. Our findings suggest a distinct interplay between ROS and epigenetic remodeling that leads to sustained cardiac contractile dysfunction in growing and young adult offspring following maternal ENM inhalation exposure.
纳米二氧化钛(nano-TiO)是应用最广泛的工程纳米材料(ENMs)之一。然而,关于母体吸入 ENM 暴露对妊娠期胎儿生长的影响,人们知之甚少。据报道,ENM 吸入暴露会降低线粒体生物能学和心脏功能,但负责的机制尚不清楚。由于 ENM 吸入暴露,活性氧(ROS)增加,但尚不清楚它们是否影响胎儿重编程。本研究的目的是确定母体吸入 ENM 暴露是否会影响后代心脏发育和表观遗传重塑。
从妊娠第 5 天(GD 5)开始,将怀孕的 FVB 母鼠暴露于浓度为 12.09±0.26mg/m 的纳米 TiO 气溶胶中,每天 6 小时,共 6 天,不连续进行。气溶胶粒径分布测量表明空气动力学计数中值直径(CMD)为 156nm,几何标准偏差(GSD)为 1.70。超声心动图成像用于评估母体、胎儿(GD 15)和幼鼠(11 周)动物的心脏功能。评估了电子传递链(ETC)复合物活性、线粒体大小、复杂性和呼吸作用,以及 5-甲基胞嘧啶、Dnmt1 蛋白表达和 Hif1α 活性。心脏功能分析显示左心室质量增加 43%,胎儿心输出量减少 25%,幼鼠心脏缩短率减少 18%。在胎儿幼仔中,过氧化氢(HO)水平显著增加(~10 倍),抗氧化酶磷脂氢过氧化物谷胱甘肽过氧化物酶(GPx4)的表达减少。ETC 复合物活性 IV 在胎儿和幼鼠心脏线粒体中分别减少了 68%和 46%。暴露后,胎儿幼仔的 DNA 甲基化显著增加,同时 Hif1α 活性和 Dnmt1 蛋白表达增加。母体暴露后,在胎儿和幼鼠阶段均观察到线粒体超微结构增大,包括大小增加。
母体吸入纳米 TiO 会对心脏功能产生不良影响,这与胎儿后代中 HO 水平升高和 Hif1α/Dnmt1 调节轴失调有关。我们的研究结果表明,ROS 和表观遗传重塑之间存在明显的相互作用,导致母体吸入 ENM 暴露后,生长中和幼鼠后代的心脏收缩功能持续受损。
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