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首页> 外文期刊>Journal of cell biology >Formation and dissociation of proteasome storage granules are regulated by cytosolic pH
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Formation and dissociation of proteasome storage granules are regulated by cytosolic pH

机译:蛋白酶体贮藏颗粒的形成和解离受细胞质pH值的调节

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摘要

The 26S proteasome is the major protein degradation machinery of the cell and is regulated at many levels. One mode of regulation involves accumulation of proteasomes in proteasome storage granules (PSGs) upon glucose depletion. Using a systematic robotic screening approach in yeast, we identify trans-acting proteins that regulate the accumulation of proteasomes in PSGs. Our dataset was enriched for subunits of the vacuolar adenosine triphosphatase (V-ATPase) complex, a proton pump required for vacuole acidification. We show that the impaired ability of V-ATPase mutants to properly govern intracellular pH affects the kinetics of PSG formation. We further show that formation of other protein aggregates upon carbon depletion also is triggered in mutants with impaired activity of the plasma membrane proton pump and the V-ATPase complex. We thus identify cytosolic pH as a specific cellular signal involved both in the glucose sensing that mediates PSG formation and in a more general mechanism for signaling carbon source exhaustion.
机译:26S蛋白酶体是细胞的主要蛋白质降解机制,并在许多水平受到调控。一种调节模式涉及在葡萄糖耗竭时蛋白酶体在蛋白酶体储存颗粒(PSG)中的积累。在酵母中使用系统的机器人筛选方法,我们确定了调节PSG中蛋白酶体积累的反式作用蛋白。我们的数据集富含液泡腺苷三磷酸酶(V-ATPase)复合物(液泡酸化所需的质子泵)的亚基。我们表明受损的V-ATPase突变体正确控制细胞内pH的能力影响PSG形成的动力学。我们进一步表明,在碳耗竭后,其他蛋白聚集体的形成也会在质膜质子泵和V-ATPase复合物活性受损的突变体中引发。因此,我们将胞质pH值确定为特定的细胞信号,参与介导PSG形成的葡萄糖传感以及信号碳源消耗的更一般机制中。

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