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AMPK phosphorylation by Ssp1 is required for proper sexual differentiation in fission yeast

机译:Ssp1的AMPK磷酸化是裂变酵母中正确性别分化所必需的

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摘要

The AMP-activated protein kinase (AMPK) is a central regulator of cellular energy homeostasis, which, in response to a fall in intracellular ATP levels, activates energy-producing pathways and inhibits energy-consuming processes. Here, we report that fission yeast cells lacking AMPK activity are unable to advance entry into mitosis in response to nitrogen starvation and cannot undergo proper G1 arrest and cell differentiation. We also show that AMPK is important in the promotion of the nuclear localization and accumulation of the Ste11 transcription factor. As in animal cells, the fission yeast CaMKK ortholog (Ssp1) phosphorylates and activates the catalytic subunit of AMPK (Ssp2) in its activation loop (Thr189) when cells are starved for nitrogen or glucose. Interestingly, we found that the phosphorylation of Ssp2 on Thr189 is required for nuclear accumulation of AMPK. Our data demonstrate the existence of a signal transduction pathway activated by nutrient starvation that triggers Ssp2 phosphorylation and AMPK redistribution from the cytoplasm to the nucleus. This pathway is important to advance fission cells into mitosis and to establish a timely pre-Start G1 cell cycle arrest for mating.
机译:AMP激活的蛋白激酶(AMPK)是细胞能量稳态的中央调节器,它响应细胞内ATP水平的下降,激活能量产生途径并抑制能量消耗过程。在这里,我们报告缺乏AMPK活性的裂变酵母细胞不能提前进入有丝分裂,以响应氮饥饿,并且不能进行适当的G1阻滞和细胞分化。我们还显示,AMPK在促进核定位和Ste11转录因子的积累中很重要。与动物细胞一样,当细胞缺乏氮或葡萄糖时,裂变酵母CaMKK直向同源物(Ssp1)磷酸化并激活AMPK(Ssp2)的催化亚基在其激活环(Thr189)中。有趣的是,我们发现Thr189上Ssp2的磷酸化是AMPK核积累所必需的。我们的数据表明存在由营养饥饿激活的信号转导通路,该信号传导通路触发Ssp2磷酸化和AMPK从细胞质到细胞核的重新分布。该途径对于使裂变细胞进入有丝分裂并建立适时的启动前G1细胞周期交配非常重要。

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