eNOS、NO 以及 ERK 和 AKT 信号在宫内生长受限羊模型中的中孕期和近足月期的激活。
eNOS, NO, and the activation of ERK and AKT signaling at mid-gestation and near-term in an ovine model of intrauterine growth restriction.
机构信息
Department of Obstetrics, University of Colorado and Health Sciences Center, Aurora, CO, USA.
出版信息
Syst Biol Reprod Med. 2010 Feb;56(1):62-73. doi: 10.3109/19396360903469307.
Intrauterine growth restriction (IUGR) is a disease responsible for neonatal morbidity and mortality and perinatal death affecting 8% of all pregnancies. In sheep, IUGR that mimics the human IUGR disease closely can be brought on by environmental hyperthermia. Endothelial nitric oxidase synthase (eNOS) and nitric oxide (NO) are important in the regulation of blood flow in the fetal-placental circulation and are modulated by several factors including hypoxia. eNOS activity is also regulated by the phosphorylation of ERK1/2 and AKT proteins in various tissues. In a hyperthermic (HT) ovine model of IUGR with systemic hypertension and increased blood flow resistance, our objective was to determine the relationship between p-ERK, p-AKT, eNOS, and NO concentrations in the placenta, uterine, and umbilical vessels at mid-gestation and near-term. Eight pregnant ewes were exposed to hyperthermic conditions for either 55 or 80 days to induce IUGR. Sheep necropsies were performed at mid-gestation and near-term for collection of placentomes, umbilical vessels, and the uterine artery. Tissues were assessed for eNOS mRNA and protein, and p-ERK and p-AKT protein. Blood was collected for NO determination at the time of necropsy. Placental insufficiency and IUGR (PI-IUGR) pregnancies demonstrated: 1) reduced placental weight at mid-gestation and reduced placental and fetal weight near-term, 2) no changes in eNOS protein concentration in the uterine artery and umbilical vessels, but an increase in NO in umbilical vein blood at both time points, 3) no significant changes in signal transduction makers (ERK/AKT) in placental tissue at mid-gestation but a significant increase near-term in cotyledon tissues, and 4) an increase in p-AKT in the uterine vessels at term. The near-term findings of increased placental p-ERK and p-AKT proteins and umbilical vein NO concentration suggest one mechanism responsible for the increase in placental eNOS previously described in this PI-IUGR model characterized by fetal systemic hypertension and abnormal umbilical artery Doppler velocimetry.
宫内生长受限(IUGR)是一种导致新生儿发病率和死亡率以及围产儿死亡的疾病,影响所有妊娠的 8%。在绵羊中,环境过热可引发类似于人类 IUGR 疾病的 IUGR。内皮型一氧化氮合酶(eNOS)和一氧化氮(NO)在胎儿胎盘循环中的血流调节中很重要,并且受到包括缺氧在内的多种因素的调节。eNOS 活性还受到 ERK1/2 和 AKT 蛋白在各种组织中的磷酸化调节。在伴有全身高血压和增加血流阻力的高热(HT)绵羊 IUGR 模型中,我们的目标是确定妊娠中期和近足月时胎盘、子宫和脐带血管中 p-ERK、p-AKT、eNOS 和 NO 浓度之间的关系。8 只怀孕的母羊暴露于 HT 条件下 55 或 80 天,以诱导 IUGR。在妊娠中期和近足月时进行绵羊尸检,以收集胎盘、脐带血管和子宫动脉。评估组织中的 eNOS mRNA 和蛋白,以及 p-ERK 和 p-AKT 蛋白。在尸检时采集血液以测定 NO。胎盘功能不全和 IUGR(PI-IUGR)妊娠表现为:1)妊娠中期胎盘重量降低,近足月时胎盘和胎儿重量降低,2)子宫动脉和脐带血管中 eNOS 蛋白浓度无变化,但在两个时间点脐带静脉血中 NO 增加,3)妊娠中期胎盘组织中信号转导标志物(ERK/AKT)无显著变化,但近足月时绒毛组织显著增加,4)足月时子宫血管中 p-AKT 增加。近足月时胎盘 p-ERK 和 p-AKT 蛋白和脐带静脉 NO 浓度的增加表明,在胎儿全身高血压和异常脐带动脉多普勒血流速度的 PI-IUGR 模型中,先前描述的胎盘 eNOS 增加的一种机制。
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