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Evidence of sexual dimorphism in the placental function with severe preeclampsia

机译:严重先兆子痫的胎盘功能性二态性的证据

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摘要

Preeclampsia (PE) affects 5-8% of pregnancies and is responsible for 18% of maternal deaths in the US, and for long-term complications in mother and child. PE is an inflammatory state and may influence placental function in a sex-specific manner. We determined if there is a sexual dimorphism in the placental inflammatory and apoptotic responses in preeclamptic pregnancies. Placentas were collected from normotensive and preeclamptic pregnancies with either male or female fetuses (MPE and FPE respectively) after c-section at term with no labor. Expression patterns of markers of inflammation measured by ELISA, as well as hypoxia, apoptosis and angiogenesis markers measured by Western blotting were determined in the placenta. Consistent with previous studies, an increase in inflammation, hypoxia, and apoptotic cell death was observed in PE compared to normotensive pregnancies. Levels of TNFα, IL-6 and IL-8, and HIF-1α were significantly greater, whereas the angiogenic marker VEGF was significantly reduced in MPE vs. FPE. Sexual dimorphism was also observed in the activation of cell death: the number of TUNEL-positive cells, and the expression pro-apoptotic markers PUMA and Bax being higher in MPE vs. FPE. We also found an increase in the levels of protein and DNA-binding activity of NFκB p65 in MPE vs. FPE. In summary, we show here that in preeclamptic pregnancies the placentas of males were associated with significantly higher expression of inflammatory, hypoxia and apoptotic molecules but reduced expression of a pro-angiogenic marker compared to placentas of female fetuses. We propose that the transcription factor NFκB p65 might, at least partially, be involved in sexual dimorphism during PE.
机译:子痫前期(PE)影响5-8%的怀孕,在美国造成18%的孕产妇死亡以及母亲和儿童的长期并发症。 PE是一种炎症状态,可能以性别特异性方式影响胎盘功能。我们确定先兆子痫孕妇的胎盘炎症和凋亡反应中是否存在性二态性。足月无剖宫产后,从血压正常和先兆子痫孕妇的男女胎(分别为MPE和FPE)中收集胎盘。在胎盘中测定通过ELISA测量的炎症标志物的表达模式,以及通过蛋白质印迹测量的缺氧,凋亡和血管生成标志物。与先前的研究一致,与正常血压妊娠相比,PE的炎症,缺氧和凋亡细胞死亡增加。 MPE与FPE相比,TNFα,IL-6,IL-8和HIF-1α的水平明显更高,而血管生成标记VEGF则显着降低。在MPE相对于FPE中,在细胞死亡的激活中也观察到了性别二态性:TUNEL阳性细胞的数量,表达促凋亡标记物PUMA和Bax更高。我们还发现MPE与FPE中NFκBp65的蛋白质​​和DNA结合活性水平增加。总而言之,我们在这里显示出,在子痫前期妊娠中,与女性胎儿的胎盘相比,男性的胎盘与炎症,缺氧和凋亡分子的表达明显更高,但促血管生成标记物的表达却降低。我们建议转录因子NFκBp65可能至少部分参与PE期间的性二态性。

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