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Enhancement of placental antioxidative function and P-gp expression by sodium ferulate mediated its protective effect on rat IUGR induced by prenatal tobacco/alcohol exposure

机译:阿魏酸钠增强胎盘抗氧化功能和P-gp表达介导其对产前烟酒暴露诱导的大鼠IUGR的保护作用

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摘要

This study was aimed to explore the therapeutic effect of sodium ferulate (SF) on rats with intrauterine growth retardation (IUGR), and then to clarify the corresponding mechanism. Pregnant rats were divided into normal group, tobacco/alcohol exposure group, and tobacco/alcohol + SF groups. Fetal developmental indices, placental weight, histological alteration, oxidative and antioxidative-function (e.g. MDA, SOD, CAT) and Mdr1 levels were assayed. Results showed exposure to tobacco/alcohol resulted in reduced fetal developmental indices and placental histological alteration, as well as the increased MDA content, decreased SOD and CAT activities and decreased Mdrla level. After SF treatment, fetal developmental indices, and placental weight, histological alteration, oxidative and antioxidative-function and mdrla levels were reversed. Our study indicated SF may be effective in reversing IUGR production, and its underlying mechanism may be due to enhanced placental antioxidative function and P-gp expression, which may be related to IUGR formation by tobacco/alcohol exposure.
机译:本研究旨在探讨阿魏酸钠(SF)对宫内发育迟缓(IUGR)大鼠的治疗作用,并阐明其相应的机制。妊娠大鼠分为正常组,烟/酒暴露组和烟/酒+ SF组。检测胎儿发育指数,胎盘重量,组织学改变,氧化和抗氧化功能(例如MDA,SOD,CAT)和Mdr1水平。结果显示,暴露于烟草/酒精中会导致胎儿发育指数降低和胎盘组织学改变,以及MDA含量增加,SOD和CAT活性降低以及Mdrla水平降低。 SF治疗后,胎儿发育指数,胎盘重量,组织学改变,氧化和抗氧化功能以及mdrla水平逆转。我们的研究表明,SF可能有效逆转IUGR的产生,其潜在机制可能归因于胎盘抗氧化功能和P-gp表达增强,这可能与烟草/酒精暴露引起的IUGR形成有关。

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