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Phosphorylation of eIF2α at Serine 51 Is an Important Determinant of Cell Survival and Adaptation to Glucose Deficiency

机译:eIF2α丝氨酸51的磷酸化是细胞存活和适应葡萄糖缺乏的重要决定因素。

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Various forms of stress induce pathways that converge on the phosphorylation of the alpha (α) subunit of eukaryotic translation initiation factor eIF2 at serine 51 (S51), a modification that results in a global inhibition of protein synthesis. In many cases eIF2α phosphorylation is a biological response that facilitates cells to cope with stressful environments. Glucose deficiency, an important form of stress, is associated with an induction of apoptosis. Herein, we demonstrate that eIF2α phosphorylation is a key step in maintaining a balance between the life and death of a glucose-deficient cell. That is, eIF2α phosphorylation acts as a molecular switch that shifts cells from a proapoptotic to a cytoprotective state in response to prolonged glucose deficiency. This adaptation process is associated with the timely expression of proteins and activation of pathways with significant contributions to cell survival and adaptation including the X-linked inhibitor of apoptosis protein ( XIAP ). We also show that among the eIF2α kinases GCN2 plays a proapoptotic role whereas PERK and PKR play a cytoprotective one in response to glucose deficiency. Our data demonstrate that eIF2α phosphorylation is a significant determinant of survival and adaptation of glucose-deficient cells with possible important implications in biological processes that interfere with glucose metabolism.
机译:各种形式的应激诱导途径收敛于丝氨酸51(S51)的真核翻译起始因子eIF2的α(α)亚基的磷酸化,这一修饰导致蛋白质合成的整体抑制。在许多情况下,eIF2α磷酸化是一种生物学反应,可促进细胞应对压力环境。葡萄糖缺乏症(一种重要的压力形式)与细胞凋亡的诱导有关。在本文中,我们证明eIF2α磷酸化是维持葡萄糖缺乏细胞的生与死之间平衡的关键步骤。即,eIF2α磷酸化作为分子开关,响应于长期的葡萄糖缺乏而使细胞从凋亡状态转变为细胞保护状态。这种适应过程与蛋白质的及时表达和通路的激活有关,这些通路对细胞存活和适应具有重大贡献,包括X连锁的凋亡蛋白抑制剂(XIAP)。我们还显示,在eIF2α激酶中,GCN2发挥促凋亡作用,而PERK和PKR在应对葡萄糖缺乏时起细胞保护作用。我们的数据表明,eIF2α磷酸化是葡萄糖缺乏细胞存活和适应的重要决定因素,在干扰葡萄糖代谢的生物过程中可能具有重要意义。

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