首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >HOIL-1 is not required for iron-mediated IRP2 degradation in HEK293 cells
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HOIL-1 is not required for iron-mediated IRP2 degradation in HEK293 cells

机译:铁介导的IRP2在HEK293细胞中的降解不需要HOIL-1

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摘要

Iron regulatory protein 2 (IRP2) binds to iron-responsive elements (IREs) to regulate the translation and stability of mRNAs encoding several proteins involved in mammalian iron homeostasis. Increases in cellular iron stimulate the polyubiquitylation and proteasomal degradation of IRP2. One study has suggested that haem-oxidized IRP2 ubiquitin ligase-1 (HOIL-1) binds to a unique 73-amino acid (aa) domain in IRP2 in an iron-dependent manner to regulate IRP2 polyubiquitylation and degradation. Other studies have questioned the role of the 73-aa domain in iron-dependent IRP2 degradation. We investigated the potential role of HOIL-1 in the iron-mediated degradation of IRP2 in human embryonic kidney 293 (HEK293) cells. We found that transiently expressed HOIL-1 and IRP2 interact via the 73-aa domain, but this interaction is not iron-dependent, nor does it enhance the rate of IRP2 degradation by iron. In addition, stable expression of HOIL-1 does not alter the iron-dependent degradation or RNA-binding activity of endogenous IRP2. Reduction of endogenous HOIL-1 by siRNA has no affect on the iron-mediated degradation of endogenous IRP2. These data demonstrate that HOIL-1 is not required for iron-dependent degradation of IRP2 in HEK293 cells, and suggest that a HOEL-1 independent mechanism is used for IRP2 degradation in most cell types. (C) 2007 Elsevier B.V. All rights reserved.
机译:铁调节蛋白2(IRP2)与铁响应元件(IREs)结合,以调节编码参与哺乳动物铁稳态的几种蛋白质的mRNA的翻译和稳定性。细胞铁的增加会刺激IRP2的多泛素化和蛋白酶体降解。一项研究表明,血红素氧化的IRP2泛素连接酶1(HOIL-1)以铁依赖的方式与IRP2中独特的73个氨基酸(aa)结构域结合,以调节IRP2的多泛素化和降解。其他研究质疑73-aa结构域在铁依赖性IRP2降解中的作用。我们调查了HOIL-1在人类胚胎肾293(HEK293)细胞中铁介导的IRP2降解中的潜在作用。我们发现,瞬时表达的HOIL-1和IRP2通过73-aa结构域相互作用,但是这种相互作用不是铁依赖性的,也不增强铁对IRP2的降解速率。此外,HOIL-1的稳定表达不会改变内源性IRP2的铁依赖性降解或RNA结合活性。 siRNA还原内源性HOIL-1对铁介导的内源性IRP2降解没有影响。这些数据证明,HOIL-1不是HEK293细胞中铁依赖的IRP2降解所必需的,并且表明在大多数细胞类型中,HOEL-1独立的机制可用于IRP2降解。 (C)2007 Elsevier B.V.保留所有权利。

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