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首页> 外文期刊>Nature Communications >Lineage marker synchrony in hematopoietic genealogies refutes the PU.1/GATA1 toggle switch paradigm
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Lineage marker synchrony in hematopoietic genealogies refutes the PU.1/GATA1 toggle switch paradigm

机译:造血谱系中的谱系标记同步性驳斥了PU.1 / GATA1拨动开关范例

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Molecular regulation of cell fate decisions underlies health and disease. To identify molecules that are active or regulated during a decision, and not before or after, the decision time point is crucial. However, cell fate markers are usually delayed and the time of?decision therefore unknown. Fortunately, dividing cells induce temporal correlations in their progeny, which allow for retrospective inference of the decision time point. We present a computational method to infer decision time points from correlated marker signals in genealogies and apply it to differentiating hematopoietic stem cells. We find that myeloid lineage decisions happen generations before lineage marker onsets. Inferred decision time points?are in agreement with data from colony assay experiments. The levels of the myeloid transcription factor PU.1 do not change during, but long after the predicted lineage decision event, indicating that the PU.1/GATA1 toggle switch paradigm cannot explain the initiation of early myeloid lineage choice.
机译:细胞命运决定的分子调控是健康和疾病的基础。为了确定在决策过程中而不是在决策之前或之后处于活动状态或受调控的分子,决策时间点至关重要。但是,细胞命运标记通常会延迟,因此决定的时间未知。幸运的是,分裂的细胞在其后代中诱导出时间相关性,从而可以追溯推断决策时间点。我们提出了一种计算方法,可以从家谱中的相关标记信号中推断出决策时间点,并将其应用于分化造血干细胞。我们发现髓系谱系决定发生在谱系标记发作之前的世代。推断的决策时间点与菌落测定实验的数据一致。髓系转录因子PU.1的水平在预测的谱系决定事件期间没有发生变化,但是很长一段时间,这表明PU.1 / GATA1拨动开关范例无法解释早期髓系谱系选择的启动。

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