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首页> 外文期刊>Placenta >Determination of non-bilayer phospholipid arrangements and their antibodies in placentae and sera of patients with hypertensive disorders of pregnancy.
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Determination of non-bilayer phospholipid arrangements and their antibodies in placentae and sera of patients with hypertensive disorders of pregnancy.

机译:妊娠高血压疾病患者胎盘和血清中非双层磷脂排列及其抗体的测定。

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摘要

Studies suggest that preeclampsia (PE) originates in the placenta and is associated with deficient trophoblast invasion of spiral arteries. The direct cause remains unknown, but preeclampsia is often associated with circulating factors that can induce generalized endothelial dysfunction. Antiphospholipid antibodies (APA) in circulation are also associated with vascular diseases. Although the quantification of APA is not currently used as a prognostic of the risk of PE, studies suggest that thrombophilias play a role in PE pathogenesis. In fact, the pathology of placentae from PE and Antiphospholipid syndrome patients is similar; atherosis, thrombosis and infarction, and endothelium activation represent the pathological mechanisms. We identified a new antibody which recognizes non-bilayer phospholipid arrangements (NPA) in membrane models and in cell membranes in vivo, and which triggered an autoimmune-like disease in mice. We evaluated the presence of NPA in the placentae and in sera, and whether NPA induced NPA antibodies in patients with hypertensive disorders of pregnancy (HDP). Results showed increased levels of NPA in the syncytiotrophoblast, extravillous cytotrophoblast, syncytial knots and the amnion epithelial cell membranes of the placenta, as well as increases in NPA and NPA antibodies in sera from HDP patients, when compared with controls. This suggests that NPA derived from placenta could be one of multiple factors associated with pregnancy pathologies.
机译:研究表明先兆子痫(PE)起源于胎盘,并与滋养细胞侵袭螺旋动脉有关。直接原因仍然未知,但先兆子痫常与可诱发广泛性内皮功能障碍的循环因素有关。循环中的抗磷脂抗体(APA)也与血管疾病有关。尽管目前尚不将APA定量作为PE风险的预后指标,但研究表明,血栓形成在PE发病机理中起着重要作用。实际上,PE和抗磷脂综合征患者的胎盘病理相似。动脉粥样硬化,血栓形成和梗塞以及内皮激活代表了病理机制。我们鉴定了一种新抗体,该抗体可识别膜模型和体内细胞膜中的非双层磷脂排列(NPA),并引发小鼠自身免疫性疾病。我们评估了胎盘和血清中NPA的存在,以及NPA是否在妊娠高血压疾病(HDP)患者中诱导NPA抗体。结果显示,与对照组相比,合胞体滋养细胞,绒毛外滋养细胞,合胞体结和胎盘羊膜上皮细胞膜中NPA的含量增加,以及HDP患者血清中NPA和NPA抗体的含量增加。这表明源自胎盘的NPA可能是与妊娠病理相关的多种因素之一。

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