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Live 4D optical coherence tomography for early embryonic mouse cardiac phenotyping

机译:早期胚胎小鼠心脏表型的活4D光学相干断层扫描

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Studying embryonic mouse development is important for our understanding of normal human embryogenesis and the underlying causes of congenital defects. Our research focuses on imaging early development in the mouse embryo to specifically understand cardiovascular development using optical coherence tomography (OCT). We have previously developed imaging approaches that combine static embryo culture, OCT imaging and advanced image processing to visualize the whole live mouse embryos and obtain 4D (3D+time) cardiodynamic datasets with cellular resolution. Here, we present the study of using 4D OCT for dynamic imaging of early embryonic heart in live mouse embryos to assess mutant cardiac phenotypes during development, including a cardiac looping defect. Our results indicate that the live 4D OCT imaging approach is an efficient phenotyping tool that can reveal structural and functional cardiac defects at very early stages. Further studies integrating live embryonic cardiodynamic phenotyping with molecular and genetic approaches in mouse mutants will help to elucidate the underlying signaling defects.
机译:研究胚胎小鼠发育对于我们对正常人体胚胎发生的理解以及先天性缺陷的根本原因很重要。我们的研究侧重于使用光学相干断层扫描(OCT)的小鼠胚胎中的早期显影性地了解心血管发展。我们之前已经开发了与静态胚胎培养,OCT成像和高级图像处理结合的成像方法,以便可视化整个实时鼠标胚胎,并获得具有蜂窝分辨率的4D(3D +时间)心动力学数据集。在这里,我们介绍了使用4D OCT进行活性小鼠胚胎早期胚胎心脏动态成像的研究,以评估开发过程中的突变心脏表型,包括心脏循环缺陷。我们的结果表明,活4D OCT成像方法是一种有效的表型工具,可以在早期阶段揭示结构和功能性心脏缺陷。进一步的研究在小鼠突变体中与分子和遗传方法相结合的实时胚胎心动力学表型将有助于阐明潜在的信号传导缺陷。

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