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首页> 外文期刊>Nucleic Acids Research >Selenite targets eIF4E-binding protein-1 to inhibit translation initiation and induce the assembly of non-canonical stress granules
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Selenite targets eIF4E-binding protein-1 to inhibit translation initiation and induce the assembly of non-canonical stress granules

机译:亚硒酸盐靶向eIF4E结合蛋白1来抑制翻译起始并诱导非规范应激颗粒的组装

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摘要

Stress granules (SGs) are large cytoplasmic ribonucleoprotein complexes that are assembled when cells are exposed to stress. SGs promote the survival of stressed cells by contributing to the reprogramming of protein expression as well as by blocking pro-apoptotic signaling cascades. These cytoprotective effects implicated SGs in the resistance of cancer cells to radiation and chemotherapy. We have found that sodium selenite, a selenium compound with chemotherapeutic potential, is a potent inducer of SG assembly. Selenite-induced SGs differ from canonical mammalian SGs in their morphology, composition and mechanism of assembly. Their assembly is induced primarily by eIF4E-binding protein1 (4EBP1)-mediated inhibition of translation initiation, which is reinforced by concurrent phosphorylation of eIF2α. Selenite-induced SGs lack several classical SG components, including proteins that contribute to pro-survival functions of canonical SGs. Our results reveal a new mechanism of mammalian SG assembly and provide insights into how selenite cytotoxicity may be exploited as an anti-neoplastic therapy.
机译:应激颗粒(SGs​​)是大型细胞质核糖核蛋白复合物,当细胞受到压力时会组装。 SG通过促进蛋白质表达的重编程以及阻断促凋亡信号级联反应来促进应激细胞的存活。这些细胞保护作用将SGs牵连到癌细胞对放射线和化学疗法的抗性中。我们发现亚硒酸钠(一种具有化学治疗潜力的硒化合物)是SG组装的有效诱导剂。亚硒酸盐诱导的SGs与典型的哺乳动物SGs的形态,组成和组装机理不同。它们的组装主要是由eIF4E结合蛋白1(4EBP1)介导的翻译起始抑制诱导的,而eIF2α的同时磷酸化增强了翻译起始。亚硒酸盐诱导的SG缺乏几种经典的SG成分,包括有助于规范SG的生存功能的蛋白质。我们的研究结果揭示了哺乳动物SG组装的新机制,并提供了有关如何利用亚硒酸盐细胞毒性作为抗肿瘤疗法的见解。

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