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Serine-threonine kinases and transcription factors active in signal transduction are detected at high levels of phosphorylation during mitosis in preimplantation embryos and trophoblast stem cells

机译:在植入前胚胎和滋养层干细胞的有丝分裂过程中,在磷酸化水平高的情况下,检测到在信号转导中具有活性的丝氨酸-苏氨酸激酶和转录因子

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摘要

Serine-threonine kinases and transcription factors play important roles in the G1-S phase progression of the cell cycle. Assays that use quantitative fluorescence by immunocytochemical means, or that measure band strength during Western blot analysis, may have confused interpretations if the intention is to measure G1-S phase commitment of a small subpopulation of phosphorylated proteins, when a larger conversion of the same population of proteins can occur during late G2 and M phases. In mouse trophoblast stem cells (TSC), a human placental cell line (HTR), and/or mouse preimplantation embryos, 8/19 serine-threonine and tyrosine kinases, 3/8 transcription factors, and 8/14 phospho substrate and miscellaneous proteins were phosphorylated at higher levels in M phase than in interphase. Most phosphoproteins appeared to associate with the spindle complex during M phase, but one (p38MAPK) associated with the spindle pole and five (Cdx2, MEK1, 2, p27, and RSK1) associated with the DNA. Phosphorylation was detected throughout apparent metaphase, anaphase and telophase for some proteins, or for only one of these segments for others. The phosphorylation was from 2.1- to 6.2-fold higher during M phase compared with interphase. These data suggest that, when planning and interpreting quantitative data and perturbation experiments, consideration must be given to the role of serine-threonine kinases and transcription factors during decision making in M phase as well as in G1-S phase.
机译:丝氨酸-苏氨酸激酶和转录因子在细胞周期的G1-S期进程中起重要作用。如果要测量少量磷酸化蛋白亚群的G1-S期定位,而同一群体的转化率较大,则通过免疫细胞化学方法使用定量荧光或在Western印迹分析过程中测量条带强度的测定可能会有混淆的解释。蛋白质可能在G2和M期后期发生。在小鼠滋养层干细胞(TSC),人胎盘细胞系(HTR)和/或小鼠植入前胚胎中,有8/19丝氨酸-苏氨酸和酪氨酸激酶,3/8转录因子以及8/14磷酸底物和其他蛋白质M相中的磷酸化水平高于中间相。大多数磷蛋白似乎在M期与纺锤体复合物缔合,但一种(p38MAPK)与纺锤体极相关,五种(Cdx2,MEK1、2,p27和RSK1)与DNA缔合。在某些蛋白质的整个明显中期,后期和末期都检测到磷酸化,而对于其他蛋白质,仅检测到其中一个片段的磷酸化。与中间相相比,M相期间的磷酸化高2.1-6.2倍。这些数据表明,在计划和解释定量数据和扰动实验时,必须考虑在M期以及G1-S期决策过程中丝氨酸-苏氨酸激酶和转录因子的作用。

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