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New Hierarchical Phosphorylation Pathway of the Translational Repressor eIF4E-binding Protein 1 (4E-BP1) in Ischemia-Reperfusion Stress

机译：缺血再灌注应激中翻译抑制基因eIF4E结合蛋白1（4E-BP1）的新的分层磷酸化途径。

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Eukaryotic initiation factor (eIF) 4E-binding protein 1 (4E-BP1) is a translational repressor that is characterized by its capacity to bind specifically to eIF4E and inhibit its interaction with eIF4G. Phosphorylation of 4E-BP1 regulates eIF4E availability, and therefore, cap-dependent translation, in cell stress. This study reports a physiological study of 4E-BP1 regulation by phosphorylation using control conditions and a stress-induced translational repression condition, ischemia-reperfusion (IR) stress, in brain tissue. In control conditions, 4E-BP1 was found in four phosphorylation states that were detected by two-dimensional gel electrophoresis and Western blotting, which corresponded to Thr⁶⁹-phosphorylated alone, Thr⁶⁹- and Thr³⁶/Thr⁴⁵-phosphorylated, all these plus Ser⁶⁴ phosphorylation, and dephosphorylation of the sites analyzed. In control or IR conditions, no Thr³⁶/Thr⁴⁵ phosphorylation alone was detected without Thr⁶⁹ phosphorylation, and neither was Ser⁶⁴ phosphorylation without Thr³⁶/Thr⁴⁵/Thr⁶⁹ phosphorylation detected. Ischemic stress induced 4E-BP1 dephosphorylation at Thr⁶⁹, Thr³⁶/Thr⁴⁵, and Ser⁶⁴ residues, with 4E-BP1 remaining phosphorylated at Thr⁶⁹ alone or dephosphorylated. In the subsequent reperfusion, 4E-BP1 phosphorylation was induced at Thr³⁶/Thr⁴⁵ and Ser⁶⁴, in addition to Thr⁶⁹. Changes in 4E-BP1 phosphorylation after IR were according to those found for Akt and mammalian target of rapamycin (mTOR) kinases. These results demonstrate a new hierarchical phosphorylation for 4E-BP1 regulation in which Thr⁶⁹ is phosphorylated first followed by Thr³⁶/Thr⁴⁵ phosphorylation, and Ser⁶⁴ is phosphorylated last. Thr⁶⁹ phosphorylation alone allows binding to eIF4E, and subsequent Thr³⁶/Thr⁴⁵ phosphorylation was sufficient to dissociate 4E-BP1 from eIF4E, which led to eIF4E-4G interaction. These data help to elucidate the physiological role of 4E-BP1 phosphorylation in controlling protein synthesis.

机译：真核起始因子（eIF）4E结合蛋白1（4E-BP1）是一种翻译阻遏物，其特征在于其与eIF4E特异性结合并抑制其与eIF4G相互作用的能力。 4E-BP1的磷酸化调节eIF4E的可用性，从而调节细胞应激中的帽依赖性翻译。这项研究报告了在大脑组织中使用控制条件和应激诱导的翻译抑制条件（缺血再灌注（IR）应激）通过磷酸化调节4E-BP1的生理研究。在对照条件下，通过二维凝胶电泳和Western blotting检测到4E-BP1处于四个磷酸化状态，分别对应于Thr ^{69 -磷酸化，Thr ^{69 -和Thr ^{36 / Thr ^{45 -磷酸化，所有这些加上Ser ^{64 磷酸化，以及所分析位点的去磷酸化。在对照或红外条件下，未检测到没有Thr ^{69 磷酸化的Thr ^{36 / Thr ^{45 磷酸化，Ser ^{64均未检测到磷酸化，未检测到Thr ^{36 / Thr ^{45 / Thr ^{69 磷酸化。缺血应激在Thr ^{69 ，Thr ^{36 / Thr ^{45 和Ser ^{64 残基处诱导4E-BP1脱磷酸， 4E-BP1仅在Thr ^{69 处被磷酸化或被去磷酸化。在随后的再灌注中，除了Thr ^{69以外，还在Thr ^{36 / Thr ^{45 和Ser ^{64 诱导了4E-BP1磷酸化。。 IR后4E-BP1磷酸化的变化与Akt和雷帕霉素（mTOR）激酶的哺乳动物靶点的发现一致。这些结果证明了4E-BP1调节的新的层次化磷酸化，其中首先对Thr ^{69 进行磷酸化，然后对Thr ^{36 / Thr ^{45 进行磷酸化， Ser ^{64 最后被磷酸化。单独的Thr ^{69 磷酸化使其与eIF4E结合，随后的Thr ^{36 / Thr ^{45 磷酸化足以使4E-BP1与eIF4E分离，从而导致与eIF4E-4G交互。这些数据有助于阐明4E-BP1磷酸化在控制蛋白质合成中的生理作用。}}}}}}}}}}}}}}}}}}}}}}}}}}}}

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期刊名称 The Journal of Biological Chemistry
作者
María I. Ayuso; Macarena Hernández-Jiménez; María E. Martín; Matilde Salinas; Alberto Alcázar;
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作者单位

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年(卷),期 2010(285),45
年度 2010
页码 34355–34363
总页数 9
原文格式 PDF
正文语种
中图分类分子生物学;
关键词
Akt PKB Ischemia mTOR Translation Initiation Factors Translation Regulation 4E-BP1 Phosphorylation 4E-binding Proteins eIF4;

机译：Akt PKB;缺血;mTOR;翻译起始因子;翻译调控;4E-BP1磷酸化;4E结合蛋白;eIF4;

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专利

1. New Hierarchical Phosphorylation Pathway of the Translational Repressor eIF4E-binding Protein 1 (4E-BP1) in Ischemia-Reperfusion Stress [J] . María I. Ayuso, Macarena Hernández-Jiménez, María Martín, The Journal of biological chemistry . 2010,第期

机译：翻译阻遏物EIF4E结合蛋白1（4E-BP1）的新分层磷酸化途径在缺血再灌注应激中
2. Regulation of the phosphorylation and integrity of protein synthesis initiation factor eIF4GI and the translational repressor 4E-BP1 by p53 [J] . Constantina Constantinou, Michael J Clemens Oncogene . 2005,第30期

机译：p53对蛋白质合成起始因子eIF4GI和翻译阻遏物4E-BP1磷酸化和完整性的调节
3. Cell cycle-dependent phosphorylation of the translational repressor eIF-4E binding protein-1 (4E-BP1) [J] . Heesom KJ, Gampel A, Mellor H, Current Biology: CB . 2001,第17期

机译：翻译抑制因子eIF-4E结合蛋白1（4E-BP1）的细胞周期依赖性磷酸化
4. Ambiguous Protein Phosphorylation Site Assignment Due to Competing Fragmentation Pathways and Gas-Phase Rearrangements in Peptides Containing Multiple Potential Phosphorylation Sites [C] . Amanda M. Palumbo, Jetze J. Tepe, Gavin E. Reid ASMS Conference on Mass Spectrometry and Allied Topics . 2008

机译：由于含有多个潜在磷酸化位点的肽的竞争碎片途径和气相重排，含糊不清蛋白质磷酸化位点分配
5. Investigation of Inducible Mitogen and Stress Activated Protein Kinase 1 (MSK1) and Histone H3 Phosphorylation by the RAS-MAPK Pathway in Cancer Cells. [D] . Espino, Paula. 2010

机译：通过癌细胞中的RAS-MAPK途径研究诱导型丝裂原和应激激活的蛋白激酶1（MSK1）和组蛋白H3磷酸化。
6. Translational Control of Cell Fate: Availability of Phosphorylation Sites on Translational Repressor 4E-BP1 Governs Its Proapoptotic Potency [O] . Shunan Li, Nahum Sonenberg, Anne-Claude Gingras, 2002

机译：细胞命运的翻译控制：翻译阻遏物4E-BP1上的磷酸化位点的可用性控制其促凋亡能力。
7. New Hierarchical Phosphorylation Pathway of the Translational Repressor eIF4E-binding Protein 1 (4E-BP1) in Ischemia-Reperfusion Stress* [O] . Ayuso, María I., Hernández-Jiménez, Macarena, Martín, María E., 2010

机译：缺血再灌注应激中翻译阻遏物eIF4E结合蛋白1（4E-BP1）的新的分层磷酸化途径*
8. Mechanism of Action of Bacteriophage T4 Translational Repressor regA Protein. [R] . Spicer, E. K. 1992

机译：噬菌体T4翻译抑制因子rega蛋白的作用机制。

New Hierarchical Phosphorylation Pathway of the Translational Repressor eIF4E-binding Protein 1 (4E-BP1) in Ischemia-Reperfusion Stress

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