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铁反应元件的结构与功能模型。

A model for the structure and functions of iron-responsive elements.

作者信息

Hentze M W, Caughman S W, Casey J L, Koeller D M, Rouault T A, Harford J B, Klausner R D

机构信息

Cell Biology and Metabolism Branch, National Institute of Child Health and Human Development, Bethesda, MD 20892.

出版信息

Gene. 1988 Dec 10;72(1-2):201-8. doi: 10.1016/0378-1119(88)90145-x.

Abstract

Most eukaryotic cells express two proteins, whose biosynthetic rates are determined by the intracellular iron status. The genes for both these proteins, ferritin and the transferrin receptor (TfR), are regulated at the post-transcriptional level, but by entirely different mechanisms. Ferritin mRNA levels are not affected by acute changes in iron availability. Ferritin biosynthesis is regulated translationally via a defined element contained within the 5' untranslated region (UTR) of the ferritin mRNA. This element has been highly conserved during evolution and has been termed an iron-responsive element (IRE). In contrast to ferritin, the regulation of TfR biosynthesis is mirrored by equivalent changes in TfR mRNA levels. The genetic information for this regulation is mostly located in the region of the gene encoding the 3' UTR of the TfR mRNA. Five elements that closely resemble the ferritin IRE are contained within the region which is critical for TfR regulation. The IRE is suggested to function by forming a specific stem-loop structure that interacts with a transacting factor in an iron-dependent fashion. We present a model that accommodates the mediation of distinct post-transcriptional regulatory phenomena via IREs.

摘要

大多数真核细胞表达两种蛋白质,其生物合成速率由细胞内铁状态决定。这两种蛋白质,即铁蛋白和转铁蛋白受体(TfR)的基因,在转录后水平受到调控,但调控机制完全不同。铁蛋白mRNA水平不受铁供应急性变化的影响。铁蛋白生物合成通过铁蛋白mRNA 5'非翻译区(UTR)内包含的一个特定元件在翻译水平上受到调控。该元件在进化过程中高度保守,被称为铁反应元件(IRE)。与铁蛋白相反,TfR生物合成的调控与TfR mRNA水平的相应变化呈镜像关系。这种调控的遗传信息大多位于编码TfR mRNA 3'UTR的基因区域内。在对TfR调控至关重要的区域内包含五个与铁蛋白IRE非常相似的元件。IRE被认为通过形成一种特定的茎环结构发挥作用,该结构以铁依赖的方式与一种反式作用因子相互作用。我们提出了一个模型,该模型通过IRE介导不同的转录后调控现象。

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