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Pomegranate Juice Supplementation Alters Utero-Placental Vascular Function and Fetal Growth in the eNOS−/− Mouse Model of Fetal Growth Restriction

机译:石榴汁补充剂在胎儿生长受限的eNOS-/-小鼠模型中改变子宫胎盘血管功能和胎儿生长

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摘要

The eNOS−/− mouse provides a well-characterized model of fetal growth restriction (FGR) with altered uterine and umbilical artery function and reduced utero- and feto-placental blood flow. Pomegranate juice (PJ), which is rich in antioxidants and bioactive polyphenols, has been posited as a beneficial dietary supplement to promote cardiovascular health. We hypothesized that maternal supplementation with PJ will improve uterine and umbilical artery function and thereby enhance fetal growth in the eNOS−/− mouse model of FGR. Wild type (WT, C57Bl/6J) and eNOS−/− mice were supplemented from E12.5-18.5 with either PJ in their drinking water or water alone. At E18.5 uterine (UtA) and umbilical (UmbA) arteries were isolated for study of vascular function, fetuses and placentas were weighed and fetal biometric measurements taken. PJ supplementation significantly increased UtA basal tone (both genotypes) and enhanced phenylephrine-induced contraction in eNOS−/− but not WT mice. Conversely PJ significantly reduced UtA relaxation in response to both acetylcholine (Ach) and sodium nitroprusside (SNP), endothelium dependent and independent vasodilators respectively from WT but not eNOS−/− mice. UmbA sensitivity to U46619-mediated contraction was increased by PJ supplementation in WT mice; PJ enhanced contraction and relaxation of UmbA to Ach and SNP respectively in both genotypes. Contrary to our hypothesis, the changes in artery function induced by PJ were not associated with an increase in fetal weight. However, PJ supplementation reduced litter size and fetal abdominal and head circumference in both genotypes. Collectively the data do not support maternal PJ supplementation as a safe or effective treatment for FGR.
机译:eNOS -/-小鼠提供了一个特征明确的胎儿生长受限(FGR)模型,其子宫和脐动脉功能改变,子宫和胎盘胎血流量降低。石榴汁(PJ)富含抗氧化剂和生物活性多酚,被认为是有益饮食的补充品,可促进心血管健康。我们假设母体补充PJ将改善FGR的eNOS -// 小鼠模型中的子宫和脐动脉功能,从而增强胎儿的生长。从E12.5-18.5中向野生型(WT,C57Bl / 6J)和eNOS -/-小鼠补充PJ或饮用水。在E18.5分离子宫(UtA)和脐带(UmbA)进行血管功能研究,称重胎儿和胎盘,并进行胎儿生物特征测量。 PJ补充剂在eNOS -/-小鼠中显着增加了UtA基础基调(两种基因型),并增强了苯肾上腺素诱导的收缩,而WT小鼠则没有。相反,PJ显着降低了分别对野生型小鼠的乙酰胆碱(Ach)和硝普钠(SNP),内皮依赖性和独立血管舒张剂的响应,而对eNOS -/-小鼠的响应却没有。在野生型小鼠中,PJ补充可增加UmbA对U46619介导的收缩的敏感性; PJ分别增强了两种基因型的UmbA对Ach和SNP的收缩和松弛。与我们的假设相反,PJ引起的动脉功能改变与胎儿体重增加无关。然而,在两种基因型中,补充PJ均可以减少产仔数以及胎儿腹部和头围。总体而言,这些数据不支持补充孕妇PJ作为FGR的安全或有效治疗方法。

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