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Identification of cardiac malformations in mice lacking Ptdsr using a novel high-throughput magnetic resonance imaging technique

机译:使用新型高通量磁共振成像技术鉴定缺乏Ptdsr的小鼠心脏畸形

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Background Congenital heart defects are the leading non-infectious cause of death in children. Genetic studies in the mouse have been crucial to uncover new genes and signaling pathways associated with heart development and congenital heart disease. The identification of murine models of congenital cardiac malformations in high-throughput mutagenesis screens and in gene-targeted models is hindered by the opacity of the mouse embryo. Results We developed and optimized a novel method for high-throughput multi-embryo magnetic resonance imaging (MRI). Using this approach we identified cardiac malformations in phosphatidylserine receptor (Ptdsr) deficient embryos. These included ventricular septal defects, double-outlet right ventricle, and hypoplasia of the pulmonary artery and thymus. These results indicate that Ptdsr plays a key role in cardiac development. Conclusions Our novel multi-embryo MRI technique enables high-throughput identification of murine models for human congenital cardiopulmonary malformations at high spatial resolution. The technique can be easily adapted for mouse mutagenesis screens and, thus provides an important new tool for identifying new mouse models for human congenital heart diseases.
机译:背景先天性心脏缺陷是导致儿童死亡的主要非感染性原因。小鼠的遗传研究对于发现与心脏发育和先天性心脏病相关的新基因和信号通路至关重要。高通量诱变筛选和基因靶向模型中先天性心脏畸形的小鼠模型的识别受到小鼠胚胎的不透明性的阻碍。结果我们开发并优化了一种用于高通量多胚胎磁共振成像(MRI)的新方法。使用这种方法,我们确定了磷脂酰丝氨酸受体(Ptdsr)缺陷胚胎中的心脏畸形。这些包括室间隔缺损,双出口右心室以及肺动脉和胸腺发育不全。这些结果表明,Ptdsr在心脏发育中起关键作用。结论我们新颖的多胚胎MRI技术可在高空间分辨率下高通量鉴定人类先天性心肺畸形的鼠模型。该技术可以轻松地应用于小鼠诱变筛选,因此为鉴定人类先天性心脏病的新小鼠模型提供了重要的新工具。

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