Hypoxia Effects on Amniotic Fluid Volume

缺氧对羊水量的影响

• 批准号: 6820696
• 负责人: ROBERT A BRACE
• 金额: $ 32.73万
• 依托单位: UNIVERSITY OF CALIFORNIA, SAN DIEGO
• 依托单位国家: 美国
• 财政年份: 1998
• 资助国家: 美国
• 起止时间: 1998-07-01 至 2009-04-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6820696
• 关键词: amniotic fluid; anemia; caveolas; caveolins; disease /disorder etiology; electron microscopy; embryo /fetus hypoxia; fluid flow; gene expression; intravital microscopy; membrane permeability; oxygen; placenta disorders; placental transfer; pregnancy; radiotracer; respiratory gas; sheep; tissue /cell culture; urination disorder; vascular endothelial growth factors; vesicle /vacuole

DESCRIPTION (provided by applicant): Recent studies have shown that amniotic fluid (AF) volume is regulated by modulating the rate of intramembranous absorption and that vascular endothelial growth factor (VEGF) may play a pivotal role in this regulation. This absorption occurs against hydrostatic, concentration and experimentally induced osmotic gradients. However, the mechanisms mediating intramembranous transport as well as the regulation of intramembmnous absorption are unknown. The proposed studies utilize chronically catheterized fetal sheep to characterize intramembranous transport mechanisms and determine the underlying cellular and molecular regulation during normoxia and during 3 forms of fetal hypoxia which individually produce increased, unchanged, or reduced AF volume. We will determine the contribution of diffusion versus bulk transport to intramembranous absorption of water and solutes. These interpretations will be confirmed by measuring the intramembranous unidirectional fluxes of specific solutes in the AF to fetal and fetal to AF directions. The cellular and molecular mechanisms which regulate passive and bulk transfer through the intramembranous pathway will be determined by studying the effects of VEGF on transport in isolated amniotic membrane and amnion cells in culture. Our overall hypothesis is that intramembranous bulk flow occurs by unidirectional vesicular transport; that hypoxia augments bulk flow but not passive diffusion; and that the rate of vesicular transport is determined by the abundance and mobility of vesicles in the amnion. We further hypothesize that hypoxia augments VEGF expression which in turn regulates caveolin-1 expression and/or increases vesicle abundance and mobility. The proposed studies are important because oligohydramnios is a frequent clinical problem associated with fetal hypoxia accounting for many in utero fetal deaths due to cord compression and neonatal deaths due to respiratory distress. Polyhydramnios is associated with premature delivery and fetal diseases including anemic hypoxia. The proposed studies will lead to a dramatic improvement in our understanding of AF volume regulation under normal as well as hypoxic conditions. This knowledge will promote a rational basis for improved therapies to treat AF volume abnormalities, thereby helping to reduce fetal and neonatal morbidity and mortality.

描述（由申请人提供）：最近的研究表明，羊水（AF）量是通过调节膜内吸收速率来调节的，血管内皮生长因子（VEGF）可能在该调节中起关键作用。这种吸收发生在流体静力学、浓度和实验诱导的渗透梯度下。然而，介导膜内转运以及调节膜内吸收的机制尚不清楚。拟定的研究利用长期插管的胎羊来表征膜内转运机制，并确定在常氧和3种形式的胎儿缺氧期间的潜在细胞和分子调控，这些缺氧分别产生AF体积增加、不变或减少。我们将确定的贡献扩散与散装运输的水和溶质的膜内吸收。这些解释将通过测量特定溶质在AF至胎儿和胎儿至AF方向上的膜内单向通量来证实。通过研究VEGF对培养的分离羊膜和羊膜细胞中转运的影响，将确定通过膜内途径调节被动和批量转运的细胞和分子机制。我们的总体假设是，膜内体积流量发生单向囊泡运输;缺氧增强体积流量，但不是被动扩散;囊泡运输的速率是由羊膜中囊泡的丰度和流动性决定的。我们进一步假设，缺氧增强VEGF的表达，反过来调节小窝蛋白-1的表达和/或增加囊泡的丰度和流动性。拟定的研究很重要，因为羊水过少是一种常见的临床问题，与胎儿缺氧有关，可解释许多宫内胎儿死亡（由于脐带压迫）和新生儿死亡（由于呼吸窘迫）。羊水过多与早产和包括贫血性缺氧在内的胎儿疾病有关。拟议的研究将导致我们对正常和缺氧条件下AF容量调节的理解的显著改善。这些知识将为治疗房颤体积异常的改进疗法提供合理的基础，从而有助于降低胎儿和新生儿的发病率和死亡率。