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双侧子宫血管结扎作为小鼠宫内生长受限的模型。

Bilateral uterine vessel ligation as a model of intrauterine growth restriction in mice.

作者信息

Janot Mathilde, Cortes-Dubly Marie-Laure, Rodriguez Stéphane, Huynh-Do Uyen

机构信息

Department of Nephrology, Hypertension and Clinical Pharmacology, Inselspital, University of Bern Medical School, Bern, Switzerland.

出版信息

Reprod Biol Endocrinol. 2014 Jul 8;12:62. doi: 10.1186/1477-7827-12-62.

Abstract

BACKGROUND

Intrauterine growth restriction (IUGR) occurs in up to 10% of pregnancies and is considered as a major risk to develop various diseases in adulthood, such as cardiovascular diseases, insulin resistance, hypertension or end stage kidney disease. Several IUGR models have been developed in order to understand the biological processes linked to fetal growth retardation, most of them being rat or mouse models and nutritional models. In order to reproduce altered placental flow, surgical models have also been developed, and among them bilateral uterine ligation has been frequently used. Nevertheless, this model has never been developed in the mouse, although murine tools display multiple advantages for biological research. The aim of this work was therefore to develop a mouse model of bilateral uterine ligation as a surgical model of IUGR.

RESULTS

In this report, we describe the set up and experimental data obtained from three different protocols (P1, P2, P3) of bilateral uterine vessel ligation in the mouse. Ligation was either performed at the cervical end of each uterine horn (P1) or at the central part of each uterine horn (P2 and P3). Time of surgery was E16 (P1), E17 (P2) or E16.5 (P3). Mortality, maternal weight and abortion parameters were recorded, as well as placentas weights, fetal resorption, viability, fetal weight and size. Results showed that P1 in test animals led to IUGR but was also accompanied with high mortality rate of mothers (50%), low viability of fetuses (8%) and high resorption rate (25%). P2 and P3 improved most of these parameters (decreased mortality and improved pregnancy outcomes; improved fetal viability to 90% and 27%, respectively) nevertheless P2 was not associated to IUGR contrary to P3. Thus P3 experimental conditions enable IUGR with better pregnancy and fetuses outcomes parameters that allow its use in experimental studies.

CONCLUSIONS

Our results show that bilateral uterine artery ligation according to the protocol we have developed and validated can be used as a surgical mouse model of IUGR.

摘要

背景

宫内生长受限(IUGR)在高达10%的妊娠中出现,被认为是成年后发生各种疾病的主要风险因素,如心血管疾病、胰岛素抵抗、高血压或终末期肾病。为了理解与胎儿生长迟缓相关的生物学过程,已经开发了几种IUGR模型,其中大多数是大鼠或小鼠模型以及营养模型。为了重现胎盘血流改变,还开发了手术模型,其中双侧子宫结扎被频繁使用。然而,尽管小鼠工具在生物学研究中具有多种优势,但该模型从未在小鼠中开发过。因此,本研究的目的是开发一种双侧子宫结扎的小鼠模型作为IUGR的手术模型。

结果

在本报告中,我们描述了从小鼠双侧子宫血管结扎的三种不同方案(P1、P2、P3)中获得的设置和实验数据。结扎在每个子宫角的宫颈端(P1)或每个子宫角的中部(P2和P3)进行。手术时间为E16(P1)、E17(P2)或E16.5(P3)。记录死亡率、母体体重和流产参数,以及胎盘重量、胎儿吸收、活力、胎儿体重和大小。结果表明,试验动物中的P1导致IUGR,但同时伴有母亲的高死亡率(50%)、胎儿的低活力(8%)和高吸收率(25%)。P2和P3改善了这些参数中的大多数(降低了死亡率并改善了妊娠结局;胎儿活力分别提高到90%和27%),然而与P3相反,P2与IUGR无关。因此,P3实验条件能够实现IUGR,并具有更好的妊娠和胎儿结局参数,可用于实验研究。

结论

我们的结果表明,根据我们开发并验证的方案进行双侧子宫动脉结扎可作为IUGR的手术小鼠模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cbe2/4105874/8170f60ba2bb/1477-7827-12-62-1.jpg

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