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首页> 美国卫生研究院文献>Portland Press Open Access >Regulation of human feto-placental endothelial barrier integrity by vascular endothelial growth factors: competitive interplay between VEGF-A165a VEGF-A165b PIGF and VE-cadherin
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Regulation of human feto-placental endothelial barrier integrity by vascular endothelial growth factors: competitive interplay between VEGF-A165a VEGF-A165b PIGF and VE-cadherin

机译:血管内皮生长因子对人胎盘血管内皮屏障完整性的调节:VEGF-A165aVEGF-A165bPIGF和VE-钙黏着蛋白之间的竞争相互作用

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The human placenta nourishes and protects the developing foetus whilst influencing maternal physiology for fetal advantage. It expresses several members of the vascular endothelial growth factor (VEGF) family including the pro-angiogenic/pro-permeability VEGF-A165a isoform, the anti-angiogenic VEGF-A165b, placental growth factor (PIGF) and their receptors, VEGFR1 and VEGFR2. Alterations in the ratio of these factors during gestation and in complicated pregnancies have been reported; however, the impact of this on feto-placental endothelial barrier integrity is unknown. The present study investigated the interplay of these factors on junctional occupancy of VE-cadherin and macromolecular leakage in human endothelial monolayers and the perfused placental microvascular bed. Whilst VEGF-A165a (50 ng/ml) increased endothelial monolayer albumin permeability (P<0.0001), equimolar concentrations of VEGF-A165b (P>0.05) or PlGF (P>0.05) did not. Moreover, VEGF-A165b (100 ng/ml; P<0.001) but not PlGF (100 ng/ml; P>0.05) inhibited VEGF-A165a-induced permeability when added singly. PlGF abolished the VEGF-A165b-induced reduction in VEGF-A165a-mediated permeability (P>0.05); PlGF was found to compete with VEGF-A165b for binding to Flt-1 at equimolar affinity. Junctional occupancy of VE-cadherin matched alterations in permeability. In the perfused microvascular bed, VEGF-A165b did not induce microvascular leakage but inhibited and reversed VEGF-A165a-induced loss of junctional VE-cadherin and tracer leakage. These results indicate that the anti-angiogenic VEGF-A165b isoform does not increase permeability in human placental microvessels or HUVEC primary cells and can interrupt VEGF-A165a-induced permeability. Moreover, the interplay of these isoforms with PIGF (and s-flt1) suggests that the ratio of these three factors may be important in determining the placental and endothelial barrier in normal and complicated pregnancies.
机译:人胎盘可滋养和保护发育中的胎儿,同时影响母体的生理,从而有利于胎儿。它表达了血管内皮生长因子(VEGF)家族的几个成员,包括促血管生成/促通透性VEGF-A165a亚型,抗血管生成VEGF-A165b,胎盘生长因子(PIGF)及其受体VEGFR1和VEGFR2。据报导,这些因素在妊娠期间和复杂妊娠中的比例发生了变化。然而,这对胎儿胎盘内皮屏障完整性的影响尚不清楚。本研究调查了这些因素对人内皮单层和灌注胎盘微血管床中VE-钙黏着蛋白的结合占用和大分子渗漏的相互作用。 VEGF-A165a(50 ng / ml)增加了内皮单层白蛋白通透性(P <0.0001),而等摩尔浓度的VEGF-A165b(P> 0.05)或PlGF(P> 0.05)却没有。此外,当单独添加时,VEGF-A165b(100ng / ml; P <0.001)而不是PlGF(100ng / ml; P> 0.05)抑制VEGF-A165a诱导的通透性。 PlGF消除了VEGF-A165b介导的通透性降低(P> 0.05);发现PlGF以等摩尔亲和力与VEGF-A165b竞争结合Flt-1。 VE-钙黏着蛋白的结点占有率与通透性的变化相匹配。在灌注的微血管床中,VEGF-A165b不会诱导微血管渗漏,但会抑制和逆转VEGF-A165a诱导的连接性VE-钙粘蛋白损失和示踪剂渗漏。这些结果表明,抗血管生成的VEGF-A165b同工型不会增加人胎盘微血管或HUVEC原代细胞的通透性,并且可以中断VEGF-A165a诱导的通透性。此外,这些同工型与PIGF(和s-flt1)的相互作用表明,这三个因素的比率对于确定正常妊娠和复杂妊娠的胎盘和内皮屏障可能很重要。

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