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深入探究严重胎儿生长受限的发病机制。

Mechanistic insights into the development of severe fetal growth restriction.

机构信息

Department of Obstetrics and Gynecology, University of Colorado School of Medicine, CO, U.S.A.

出版信息

Clin Sci (Lond). 2023 Apr 26;137(8):679-695. doi: 10.1042/CS20220284.

Abstract

Fetal growth restriction (FGR), which most commonly results from suboptimal placental function, substantially increases risks for adverse perinatal and long-term outcomes. The only "treatment" that exists is delivery, which averts stillbirth but does not improve outcomes in survivors. Furthermore, the potential long-term consequences of FGR to the fetus, including cardiometabolic disorders, predispose these individuals to developing FGR in their future pregnancies. This creates a multi-generational cascade of adverse effects stemming from a single dysfunctional placenta, and understanding the mechanisms underlying placental-mediated FGR is critically important if we are to improve outcomes and overall health. The mechanisms behind FGR remain unknown. However, placental insufficiency derived from maldevelopment of the placental vascular systems is the most common etiology. To highlight important mechanistic interactions within the placenta, we focus on placental vascular development in the setting of FGR. We delve into fetoplacental angiogenesis, a robust and ongoing process in normal pregnancies that is impaired in severe FGR. We review cellular models of FGR, with special attention to fetoplacental angiogenesis, and we highlight novel integrin-extracellular matrix interactions that regulate placental angiogenesis in severe FGR. In total, this review focuses on key developmental processes, with specific focus on the human placenta, an underexplored area of research.

摘要

胎儿生长受限(FGR)主要由胎盘功能不全引起,会显著增加围产期和长期不良结局的风险。目前唯一的“治疗”方法是分娩,这可以避免死产,但不能改善幸存者的结局。此外,FGR 给胎儿带来的潜在长期后果,包括心脏代谢紊乱,使这些个体在未来的妊娠中易发生 FGR。这就产生了一个由单个功能失调的胎盘引起的多代级联不良影响,了解胎盘介导的 FGR 的机制对于改善结局和整体健康至关重要。FGR 的机制尚不清楚。然而,源自胎盘血管系统发育不良的胎盘功能不全是最常见的病因。为了突出胎盘内重要的机制相互作用,我们重点关注 FGR 背景下的胎盘血管发育。我们深入研究了胎-胎盘血管生成,这是正常妊娠中一个强大且持续的过程,但在严重的 FGR 中受到损害。我们综述了 FGR 的细胞模型,特别关注胎-胎盘血管生成,并强调了调节严重 FGR 中胎盘血管生成的新型整合素-细胞外基质相互作用。总的来说,这篇综述侧重于关键的发育过程,特别关注人类胎盘,这是一个研究不足的领域。

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