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eIF4E 结合蛋白对具有不同 5'-UTR 二级结构的 mRNAs 的调节:蛋白质-mRNA 相互作用的一个组成部分的多静电模型。

eIF4E-binding protein regulation of mRNAs with differential 5'-UTR secondary structure: a polyelectrostatic model for a component of protein-mRNA interactions.

机构信息

Faculty of Life Sciences, University of Manchester, Manchester Interdisciplinary Biocentre, 131 Princess Street, Manchester M1 7DN, UK.

出版信息

Nucleic Acids Res. 2012 Sep;40(16):7666-75. doi: 10.1093/nar/gks511. Epub 2012 Jun 20.

Abstract

Control of translation in eukaryotes is complex, depending on the binding of various factors to mRNAs. Available data for subsets of mRNAs that are translationally up- and down-regulated in yeast eIF4E-binding protein (4E-BP) deletion mutants are coupled with reported mRNA secondary structure measurements to investigate whether 5'-UTR secondary structure varies between the subsets. Genes with up-regulated translational efficiencies in the caf20Δ mutant have relatively high averaged 5'-UTR secondary structure. There is no apparent wide-scale correlation of RNA-binding protein preferences with the increased 5'-UTR secondary structure, leading us to speculate that the secondary structure itself may play a role in differential partitioning of mRNAs between eIF4E/4E-BP repression and eIF4E/eIF4G translation initiation. Both Caf20p and Eap1p contain stretches of positive charge in regions of predicted disorder. Such regions are also present in eIF4G and have been reported to associate with mRNA binding. The pattern of these segments, around the canonical eIF4E-binding motif, varies between each 4E-BP and eIF4G. Analysis of gene ontology shows that yeast proteins containing predicted disordered segments, with positive charge runs, are enriched for nucleic acid binding. We propose that the 4E-BPs act, in part, as differential, flexible, polyelectrostatic scaffolds for mRNAs.

摘要

真核生物的翻译控制很复杂,取决于各种因素与 mRNA 的结合。对在酵母 eIF4E 结合蛋白(4E-BP)缺失突变体中翻译上调和下调的 mRNA 亚群的已有数据,与报告的 mRNA 二级结构测量结果相结合,研究了 5'-UTR 二级结构是否在这些亚群之间存在差异。在 caf20Δ 突变体中翻译效率上调的基因具有相对较高的平均 5'-UTR 二级结构。RNA 结合蛋白偏好性与增加的 5'-UTR 二级结构之间没有明显的广泛相关性,这使我们推测二级结构本身可能在 mRNAs 在 eIF4E/4E-BP 抑制和 eIF4E/eIF4G 翻译起始之间的差异分配中起作用。Caf20p 和 Eap1p 在预测的无序区域都含有一段正电荷。eIF4G 中也存在这种区域,并且据报道与 mRNA 结合有关。这些片段的模式,围绕着典型的 eIF4E 结合基序,在每个 4E-BP 和 eIF4G 之间都有所不同。对基因本体论的分析表明,含有预测无序片段和正电荷的酵母蛋白富含核酸结合。我们提出 4E-BPs 部分充当 mRNA 的差异、灵活、多静电支架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b50b/3439904/09a6c2f50c91/gks511f1.jpg

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