Preeclampsia: From Inflammation to Immunoregulation.

IF 3 Q2 Medicine Clinical Medicine Insights-Blood Disorders Pub Date : 2018-01-10 eCollection Date: 2018-01-01 DOI:10.1177/1179545X17752325
Denise C Cornelius
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引用次数: 114

Abstract

Preeclampsia (PE) affects 5% to 7% of pregnant women each year worldwide, accounts for up to 18% of maternal deaths in the United States each year, and is the number 1 cause of premature births. Preeclampsia is associated with hypertension after the 20th week of gestation with or without proteinuria, in conjunction with fetal growth restriction, maternal endothelial dysfunction, and chronic immune activation. The mechanisms leading to the development of PE are unclear. However, it is thought that shallow trophoblast invasion and insufficient remodeling of uterine spiral arteries result in placental ischemia. Consequently, an immune imbalance characterized by increases in proinflammatory CD4+ T cells and cytokines along with decreases in regulatory T cells and anti-inflammatory cytokines occurs. This imbalance leads to chronic inflammation and ensuing oxidative stress, proinflammatory cytokines, and autoantibodies. Studies performed in our laboratories, using the Reduced Uterine Perfusion Pressure (RUPP) rat model of placental ischemia, have demonstrated a role for this immune imbalance to mediate PE pathophysiology and identified potential mechanisms of immunoregulation that may be of benefit in the treatment of PE. Therefore, the purpose of this commentary is to review studies demonstrating the positive effects of immunoregulatory factors in the RUPP rat model of PE. Restoration of the immune balance in PE may be a potential strategy for the development of therapeutic interventions that could improve maternal and fetal outcomes associated with this maternal syndrome.

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子痫前期:从炎症到免疫调节。
先兆子痫(PE)每年影响全球5%至7%的孕妇,占美国每年孕产妇死亡人数的18%,是早产的第一大原因。先兆子痫与妊娠20周后伴有蛋白尿或无蛋白尿的高血压有关,并伴有胎儿生长受限、母体内皮功能障碍和慢性免疫激活。导致PE发展的机制尚不清楚。然而,滋养细胞浸润较浅和子宫螺旋动脉重构不足被认为是导致胎盘缺血的原因。因此,以促炎CD4+ T细胞和细胞因子的增加以及调节性T细胞和抗炎细胞因子的减少为特征的免疫失衡发生。这种不平衡导致慢性炎症和随后的氧化应激、促炎细胞因子和自身抗体。在我们的实验室中,使用子宫灌注压降低(RUPP)大鼠胎盘缺血模型进行的研究已经证明了这种免疫失衡介导PE病理生理的作用,并确定了可能有益于PE治疗的免疫调节潜在机制。因此,本评论的目的是回顾证明免疫调节因子在RUPP大鼠PE模型中的积极作用的研究。恢复PE的免疫平衡可能是开发治疗干预措施的潜在策略,可以改善与该母体综合征相关的母体和胎儿结局。
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来源期刊
CiteScore
3.70
自引率
0.00%
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审稿时长
8 weeks
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