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使用高频超声(30/45兆赫兹)系统对胎鼠进行心血管成像

Fetal Mouse Cardiovascular Imaging Using a High-frequency Ultrasound (30/45MHZ) System.

作者信息

Touma Marlin

机构信息

Neonatal/Congenital Heart Laboratory, Cardiovascular Research Laboratory, David Geffen School of Medicine, University of California, Los Angeles; Children's Discovery and Innovation Institute, Department of Pediatrics, David Geffen School of Medicine, University of California, Los Angeles;

出版信息

J Vis Exp. 2018 May 5(135):57210. doi: 10.3791/57210.

Abstract

Congenital heart defects (CHDs) are the most common cause of childhood morbidity and early mortality. Prenatal detection of the underlying molecular mechanisms of CHDs is crucial for inventing new preventive and therapeutic strategies. Mutant mouse models are powerful tools to discover new mechanisms and environmental stress modifiers that drive cardiac development and their potential alteration in CHDs. However, efforts to establish the causality of these putative contributors have been limited to histological and molecular studies in non-survival animal experiments, in which monitoring the key physiological and hemodynamic parameters is often absent. Live imaging technology has become an essential tool to establish the etiology of CHDs. In particular, ultrasound imaging can be used prenatally without surgically exposing the fetuses, allowing maintaining their baseline physiology while monitoring the impact of environmental stress on the hemodynamic and structural aspects of cardiac chamber development. Herein, we use the High-Frequency Ultrasound (30/45) system to examine the cardiovascular system in fetal mice at E18.5 in utero at the baseline and in response to prenatal hypoxia exposure. We demonstrate the feasibility of the system to measure cardiac chamber size, morphology, ventricular function, fetal heart rate, and umbilical artery flow indices, and their alterations in fetal mice exposed to systemic chronic hypoxia in utero in real time.

摘要

先天性心脏缺陷(CHD)是儿童发病和早期死亡的最常见原因。产前检测CHD的潜在分子机制对于发明新的预防和治疗策略至关重要。突变小鼠模型是发现驱动心脏发育的新机制和环境应激调节因子及其在CHD中潜在改变的有力工具。然而,在非存活动物实验中,确定这些假定因素因果关系的努力仅限于组织学和分子研究,其中往往缺乏对关键生理和血流动力学参数的监测。活体成像技术已成为确定CHD病因的重要工具。特别是,超声成像可在产前使用,无需手术暴露胎儿,从而在监测环境应激对心腔发育的血流动力学和结构方面的影响时保持其基线生理状态。在此,我们使用高频超声(30/45)系统在子宫内E18.5时对胎儿小鼠的心血管系统进行基线检查,并观察产前低氧暴露后的反应。我们证明了该系统能够实时测量心腔大小、形态、心室功能、胎儿心率和脐动脉血流指数,以及在子宫内暴露于全身性慢性低氧的胎儿小鼠中的这些参数变化。

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