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滋养细胞 plugs:对子宫胎盘血液动力学和螺旋动脉重塑的影响。

Trophoblast plugs: impact on utero-placental haemodynamics and spiral artery remodelling.

机构信息

Department of Obstetrics and Gynaecology, Faculty of Medical and Health Sciences, The University of Auckland, Private Bag 92019, Auckland Mail Centre, Auckland 1142, New Zealand.

Auckland Bioengineering Institute, The University of Auckland, Private Bag 92019, Auckland Mail Centre, Auckland 1142, New Zealand.

出版信息

Hum Reprod. 2018 Aug 1;33(8):1430-1441. doi: 10.1093/humrep/dey225.

Abstract

STUDY QUESTION

How does trophoblast plugging impact utero-placental haemodynamics?

SUMMARY ANSWER

Physiological trophoblast plug structures are dense enough to restrict flow of oxygenated blood to the intervillous space (IVS) in the first trimester, and result in a shear stress environment upstream of the plugs that promotes spiral artery remodelling.

WHAT IS KNOWN ALREADY

Trophoblast plugging of the uterine spiral arteries is thought to be the dominant factor restricting the flow of oxygenated maternal blood to the placenta in the first trimester of pregnancy. However, the extent of plugging, the timing of plug break up, and the impact of plug structure on pregnancy outcomes is debated.

STUDY DESIGN, SIZE, DURATION: A computational model of the uterine radial and spiral arteries, incorporating arteriovenous anastomoses was developed. The model was parameterized with our own histological data and previous literature descriptions of the dimensions of the spiral arteries, and the structural properties (porosity) of trophoblast plugs.

PARTICIPANTS/MATERIALS, SETTING, METHODS: Structural data were acquired from the literature, and supplemented by images of the spiral arteries acquired by standard thin-section 2D immunohistochemistry, and whole mount immunohistochemistry imaged in 3D by micro-CT. Computational models were solved using Matlab software, via custom written scripts.

MAIN RESULTS AND THE ROLE OF CHANCE

We confirm that physiological lengths (>0.1 mm) and porosities (0.2-0.6) of trophoblast plugs are sufficient to restrict the flow of oxygenated maternal blood flow to the placental surface. Trophoblast plugs also have important haemodynamic consequences upstream in the spiral arteries by generating shear stress conditions of <2 dyne/cm2 that promote trophoblast-induced spiral artery remodelling. Structural changes in plugs as they dislodge are likely to result in rapid increases in blood flow to the IVS, and it is likely at this stage of gestation that the major source of resistance in the utero-placental circulation transitions from the spiral arteries to the radial arteries, which then act as a the 'rate-limiting' step to IVS flow.

LIMITATIONS, REASONS FOR CAUTION: Structural descriptions of the spiral arteries, radial arteries and trophoblast plugs largely rely on 2D histological sections, or historical measurements. Increased focus on quantitatively assessing the 3D structure of the uterine arteries using more modern imaging technologies in the future will strengthen model predictions.

WIDER IMPLICATIONS OF THE FINDINGS

Our work suggests that trophoblast plugs play a previously under-appreciated role in regulating spiral artery remodelling in the first trimester of human pregnancy. This creates the possibility that inadequate trophoblast plugging in the first trimester may contribute to the inadequate artery remodelling observed in pregnancy pathologies such as pre-eclampsia. The incorporation of arteriovenous anastomoses in our model highlights the important influence that shunted blood can play in utero-placental haemodynamics, and together with the emerging role of radial arteries in regulating blood flow to the placenta, the influence of arteriovenous anastomoses on radial artery haemodynamics in normal and pathological pregnancies warrants further investigation.

STUDY FUNDING/COMPETING INTEREST(S): This research was supported by a Royal Society of New Zealand Marsden Fund award (13-UOA-032). A.R.C. is supported by a Royal Society of New Zealand Rutherford Discovery Fellowship (14-UOA-019). R.S. was supported by a Gravida (National Centre for Growth and Development) postgraduate scholarship. The authors have no conflicts of interest.

TRIAL REGISTRATION NUMBER

N/A.

摘要

研究问题

滋养细胞栓子如何影响子宫胎盘血液动力学?

总结答案

生理滋养细胞栓结构足够致密,可在妊娠早期限制含氧血液流入绒毛间隙(IVS),并在上游形成促使螺旋动脉重塑的剪应力环境。

已知情况

人们认为,滋养细胞栓子阻塞子宫螺旋动脉是限制妊娠早期母体含氧血液流向胎盘的主要因素。然而,栓子的阻塞程度、栓子的破裂时间以及栓子结构对妊娠结局的影响仍存在争议。

研究设计、规模、持续时间:开发了一个包含动静脉吻合的子宫放射状和螺旋动脉的计算模型。该模型使用我们自己的组织学数据和以前关于螺旋动脉尺寸以及滋养细胞栓子结构特性(孔隙率)的文献描述进行参数化。

参与者/材料、设置、方法:结构数据来自文献,并通过标准的 2D 免疫组织化学获取的螺旋动脉图像以及通过微 CT 在 3D 中成像的整体免疫组织化学图像进行补充。使用 Matlab 软件通过自定义编写的脚本解决计算模型。

主要结果和机会的作用

我们证实,生理长度(>0.1mm)和孔隙率(0.2-0.6)的滋养细胞栓足以限制含氧母体血流向胎盘表面的流动。滋养细胞栓在上游螺旋动脉中也具有重要的血液动力学后果,会产生<2 达因/平方厘米的剪应力条件,从而促进滋养细胞诱导的螺旋动脉重塑。随着栓子的脱落,栓子结构发生变化,可能导致 IVS 血流迅速增加,并且很可能在妊娠的这个阶段,子宫胎盘循环中的主要阻力源从螺旋动脉转移到放射状动脉,然后放射状动脉成为 IVS 血流的“限速”步骤。

局限性、谨慎的原因:螺旋动脉、放射状动脉和滋养细胞栓的结构描述主要依赖于 2D 组织学切片或历史测量。未来更多地关注使用现代成像技术定量评估子宫动脉的 3D 结构,将增强模型预测。

研究结果的更广泛意义

我们的工作表明,滋养细胞栓在调节人类妊娠早期螺旋动脉重塑中发挥了以前被低估的作用。这就产生了一种可能性,即妊娠早期滋养细胞栓不足可能导致子痫前期等妊娠病理中观察到的动脉重塑不足。我们模型中包含动静脉吻合,突出了分流血液在子宫胎盘血液动力学中的重要作用,以及正在出现的放射状动脉在调节胎盘血流中的作用,动静脉吻合对正常和病理妊娠中放射状动脉血液动力学的影响值得进一步研究。

研究资金/竞争利益:这项研究得到了新西兰皇家学会 Marsden 基金奖(13-UOA-032)的支持。ARC 得到了新西兰皇家学会 Rutherford 发现奖学金(14-UOA-019)的支持。RS 得到了 Gravida(国家生长与发育中心)研究生奖学金的支持。作者没有利益冲突。

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