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Multiscale, multimodal, and multidimensional microscopy of cardiac development

机译:多尺寸,多模式和心脏发育的多维显微镜显微镜

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In vivo fluorescence imaging of the embryonic zebrafish heart as it develops and gains function has recently become possible thanks to several breakthroughs in fast microscopy. However, because of the motion of the fast beating heart, volumetric, long term, continuous, and simultaneous characterization of subtle changes in heart morphology at the organ, tissue and cellular level, changes in heart function, or changes in local gene expression all remain major challenges. We have developed tools that aim at addressing the problem of capturing and integrating multi-modal data at different temporal and spatial scales to build a multi-dimensional model of the beating and developing heart. This paper gives an overview of techniques we developed and integrated to follow heart development, spatiotemporally confined hemodynamics, and gene expression. These tools permit quantitative characterization and will allow studying the interactions between genetic and epigenetic factors that affect cardiac development.
机译:在胚胎斑马鱼心脏的体内荧光成像中,由于快速显微镜的几个突破,最近可能成为可能的增加。然而,由于快速跳动的心脏,体积,长期,连续,同时表征器官,组织和细胞水平的细微变化,心脏功能变化,或局部基因表达的变化都仍然存在主要挑战。我们开发了旨在解决在不同时间和空间尺度上捕获和集成多模态数据的问题的工具,以构建跳动和开发心脏的多维模型。本文概述了我们开发和综合的技术,以遵循心脏发育,割型狭窄的血液动力学和基因表达。这些工具允许定量表征,并允许研究影响心脏发育的遗传和表观遗传因素之间的相互作用。

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