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Variability in beta-catenin pulse dynamics in a stochastic cell fate decision in C. elegans

机译:在C.秀丽隐杆线的随机电池命运决策中β-catenin脉冲动力学的变异性

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During development, cell fate decisions are often highly stochastic, but with the frequency of the different possible fates tightly controlled. To understand how signaling networks control the cell fate frequency of such random decisions, we studied the stochastic decision of the Caenorhabditis elegans P3.p cell to either fuse to the hypodermis or assume vulva precursor cell fate. Using time-lapse microscopy to measure the single-cell dynamics of two key inhibitors of cell fusion, the Hox gene LIN-39 and Wnt signaling through the beta-catenin BAR-1, we uncovered significant variability in the dynamics of LIN-39 and BAR-1 levels. Most strikingly, we observed that BAR-1 accumulated in a single, 1-4 h pulse at the time of the P3.p cell fate decision, with strong variability both in pulse slope and time of pulse onset. We found that the time of BAR-1 pulse onset was delayed relative to the time of cell fusion in mutants with low cell fusion frequency, linking BAR-1 pulse timing to cell fate outcome. Overall, a model emerged where animal-to-animal variability in LIN-39 levels and BAR-1 pulse dynamics biases cell fate by modulating their absolute level at the time cell fusion is induced. Our results highlight that timing of cell signaling dynamics, rather than its average level or amplitude, could play an instructive role in determining cell fate.
机译:在开发期间,细胞命运决定通常是高度随机的,但是频率与不同可能的命运频率紧密控制。要了解信令网络如何控制这种随机决策的细胞命运频率,我们研究了Caenorhabdise Legans P3.P细胞的随机决定,融合给皮下注射或假设外阴前体细胞命运。使用延时显微镜测量细胞融合的两个关键抑制剂的单细胞动态,通过β-catenin bar-1来揭示HIN-Catenin Bar-1的HOX基因LIN-39和WNT信号传导,我们在LIN-39的动态中发现了显着的变化酒吧1级。最引人注目的是,我们观察到在P3.P细胞命运决策时在单一,1-4小时脉冲中累积的条形图,在脉冲斜率和脉冲发作时间内具有很强的变化。我们发现,相对于具有低电池融合频率的突变体中的细胞融合的时间,将Bar-1脉冲发作的时间延迟,将Bar-1脉冲定时连接到细胞命运结果。总的来说,诱导了诱导林-39水平和脉冲动力学在林-39水平和脉冲动力学中的动物对动物变异来偏置细胞命运的模型,诱导在时间细胞融合时调节它们的绝对水平。我们的结果强调了小区信令动态的时序,而不是其平均水平或幅度,可以在确定细胞命运中发挥作用。

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