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Spatial gradients of protein-level time delays set the pace of the traveling segmentation clock waves

机译:蛋白质水平时延的空间梯度决定了行进式分段时钟波的速度

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摘要

The vertebrate segmentation clock is a gene expression oscillator controlling rhythmic segmentation of the vertebral column during embryonic development. The period of oscillations becomes longer as cells are displaced along the posterior to anterior axis, which results in traveling waves of clock gene expression sweeping in the unsegmented tissue. Although various hypotheses necessitating the inclusion of additional regulatory genes into the core clock network at different spatial locations have been proposed, the mechanism underlying traveling waves has remained elusive. Here, we combined molecular-level computational modeling and quantitative experimentation to solve this puzzle. Our model predicts the existence of an increasing gradient of gene expression time delays along the posterior to anterior direction to recapitulate spatiotemporal profiles of the traveling segmentation clock waves in different genetic backgrounds in zebrafish. We validated this prediction by measuring an increased time delay of oscillatory Her1 protein production along the unsegmented tissue. Our results refuted the need for spatial expansion of the core feedback loop to explain the occurrence of traveling waves. Spatial regulation of gene expression time delays is a novel way of creating dynamic patterns; this is the first report demonstrating such a control mechanism in any tissue and future investigations will explore the presence of analogous examples in other biological systems.
机译:脊椎动物分段时钟是一种基因表达振荡器,可控制胚胎发育过程中椎骨节律性分段。随着细胞沿后轴到前轴的移位,振荡的周期变长,这导致时钟基因表达的行波在未分割的组织中扫过。尽管已经提出了各种假设,要求在不同的空间位置将额外的调控基因包含到核心时钟网络中,但是行波背后的机制仍然难以捉摸。在这里,我们结合了分子水平的计算模型和定量实验来解决这个难题。我们的模型预测,从后到前的方向,基因表达时间延迟的梯度会不断增加,以概括斑马鱼不同遗传背景中的行进分割时钟的时空分布。我们通过测量沿未分割组织的振荡性Her1蛋白产生的增加的时间延迟来验证此预测。我们的结果驳斥了对核心反馈回路进行空间扩展以解释行波发生的必要性。基因表达时延的空间调节是一种创建动态模式的新颖方法。这是第一份证明在任何组织中都存在这种控制机制的报告,未来的研究将探索其他生物系统中类似实例的存在。

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