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Measurement and 3D-Visualization of Cell-Cycle Length Using Double Labelling with Two Thymidine Analogues Applied in Early Heart Development

机译:细胞周期长度的测量及三维可视化在早期心脏发育使用双标配有两张胸腺嘧啶核苷类似物应用

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摘要

Organ development is a complex spatial process in which local differences in cell proliferation rate play a key role. Understanding this role requires the measurement of the length of the cell cycle at every position of the three-dimensional (3D) structure. This measurement can be accomplished by exposing the developing embryo to two different thymidine analogues for two different durations immediately followed by tissue fixation. This paper presents a method and a dedicated computer program to measure the resulting labelling indices and subsequently calculate and visualize local cell cycle lengths within the 3D morphological context of a developing organ. By applying this method to the developing heart, we show a large difference in cell cycle lengths between the early heart tube and the adjacent mesenchyme of the pericardial wall. Later in development, a local increase in cell size was found to be associated with a decrease in cell cycle length in the region where the chamber myocardium starts to develop. The combined application of halogenated-thymidine double exposure and image processing enables the automated study of local cell cycle parameters in single specimens in a full 3D context. It can be applied in a wide range of research fields ranging from embryonic development to tissue regeneration and cancer research.
机译:器官发育是一个复杂的空间过程,其中细胞增殖率的局部差异起着关键作用。要了解此角色,需要测量三维(3D)结构每个位置的细胞周期长度。可以通过将发育中的胚胎立即暴露于两种不同的胸苷类似物中两个不同的时间,然后立即进行组织固定来完成此测量。本文提出了一种方法和专用的计算机程序,用于测量所得的标记指数,并随后在发育器官的3D形态环境内计算和可视化局部细胞周期长度。通过将这种方法应用于正在发育的心脏,我们显示出早期心管与心包壁的相邻间充质之间的细胞周期长度差异很大。在发育的后期,发现细胞大小的局部增加与室心肌开始发展的区域中细胞周期长度的减少有关。卤代胸腺嘧啶双曝光和图像处理的结合应用,可以在完整的3D环境中自动研究单个样本中的局部细胞周期参数。它可以应用于从胚胎发育到组织再生和癌症研究的广泛研究领域。

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