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首页> 美国卫生研究院文献>other >Hyperoxia-mediated transcriptional activation of cytochrome P4501A1 (CYP1A1) and decreased susceptibility to oxygen-mediated lung injury in newborn mice
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Hyperoxia-mediated transcriptional activation of cytochrome P4501A1 (CYP1A1) and decreased susceptibility to oxygen-mediated lung injury in newborn mice

机译:高氧介导的细胞色素P4501A1(CYP1A1)转录激活和对氧介导的肺损伤的敏感性降低

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Hyperoxia contributes to the development of bronchopulmonary dysplasia (BPD) in premature infants. In this study, we tested the hypothesis that newborn transgenic mice carrying the human CYP1A1-Luc promoter will display transcriptional activation of the human CYP1A1 promoter in vivo upon exposure to hyperoxia, and that these mice will be less susceptible to hyperoxic lung injury and alveolar simpliFIcation than similarly exposed wild type (WT) mice. Newborn WT (CD-1) or transgenic mice carrying a 13.2 kb human CYP1A1 promoter and the luciferase (Luc) reporter gene (CYP1A1-luc) were maintained in room air or exposed to hyperoxia (85% O2) for 7–14 days. Hyperoxia exposure of CYP1A1-Luc mice for 7 and 14 days resulted in 4- and 30-fold increases, respectively, in hepatic Luc (CYP1A1) expression, compared to room air controls. In lung, hyperoxia caused a 2-fold induction of reporter Luc at 7 days, but the induction declined after 14 days. The newborn CYP1A1-Luc mice were less susceptible to lung injury and alveolar simplification than similarly exposed wild type (WT) CD-1 mice. Also, the CYP1A1-Luc mice showed increased levels of hepatic and pulmonary CYP1A1 expression and hepatic CYP1A2 activity after hyperoxia exposure. Hyperoxia also increased NADP(H) quinone reductase (NQO1) pulmonary gene expression in both CD-1 and CYP1A1-Luc mice at both time points, but this was more pronounced in the latter at 14 days. Our results support the hypothesis that hyperoxia activates the human CYP1A1 promoter in newborn mice, and that increased endogenous expression of CYP1A1 and NADP(H) quinone reductase (NQO1) contributes to the decreased susceptibilities to hyperoxic lung injury in the transgenic animals. This is the first report providing evidence of hyperoxia-mediated transcriptional activation of the human CYP1A1 promoter in newborn mice, and this in conjunction with decreased lung injury, suggests that these phenomena have important implications for BPD.
机译:高氧血症导致早产儿支气管肺发育不良(BPD)的发展。在这项研究中,我们测试了以下假设,即携带人CYP1A1-Luc启动子的新生转基因小鼠在暴露于高氧环境下将在体内显示出人CYP1A1启动子的转录激活,并且这些小鼠对高氧肺损伤和肺泡简化的敏感性较低比暴露于野生型(WT)的小鼠要多。将携带13.2 kb人类CYP1A1启动子和荧光素酶(Luc)报告基因(CYP1A1-luc)的新生WT(CD-1)或转基因小鼠在室内空气中放置或暴露于高氧(85%O2)中7-14天。与室内空气对照组相比,CYP1A1-Luc小鼠高氧暴露7天和14天分别导致肝Luc(CYP1A1)表达增加4倍和30倍。在肺中,高氧在7天时导致2倍于报告基因Luc的诱导,但在14天后诱导降低。与类似暴露的野生型(WT)CD-1小鼠相比,新生的CYP1A1-Luc小鼠对肺部损伤和肺泡简化的敏感性较低。同样,CYP1A1-Luc小鼠在高氧暴露后肝和肺CYP1A1表达水平升高,肝CYP1A2活性升高。高氧还增加了CD-1和CYP1A1-Luc小鼠在两个时间点的NADP(H)醌还原酶(NQO1)肺基因表达,但这在14天时更为明显。我们的结果支持以下假设:高氧激活新生小鼠中的人CYP1A1启动子,而CYP1A1和NADP(H)醌还原酶(NQO1)的内源性表达增加,导致转基因动物对高氧肺损伤的敏感性降低。这是第一份报告,提供了新生小鼠中人CYP1A1启动子的高氧介导的转录激活的证据,这与减少的肺损伤相结合,表明这些现象对BPD具有重要意义。

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