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哺乳动物 Lipocalin UTRs 的计算机特征分析:对其在转录后调控中作用的预测。

Characterization of mammalian Lipocalin UTRs in silico: Predictions for their role in post-transcriptional regulation.

机构信息

Departamento de Genetica, Universidad de Sevilla, Sevilla, Spain.

Instituto de Biologia y Genetica Molecular-Departamento de Bioquimica y Biologia Molecular y Fisiologia, Universidad de Valladolid-CSIC, Valladolid, Spain.

出版信息

PLoS One. 2019 Mar 6;14(3):e0213206. doi: 10.1371/journal.pone.0213206. eCollection 2019.

Abstract

The Lipocalin family is a group of homologous proteins characterized by its big array of functional capabilities. As extracellular proteins, they can bind small hydrophobic ligands through a well-conserved β-barrel folding. Lipocalins evolutionary history sprawls across many different taxa and shows great divergence even within chordates. This variability is also found in their heterogeneous tissue expression pattern. Although a handful of promoter regions have been previously described, studies on UTR regulatory roles in Lipocalin gene expression are scarce. Here we report a comprehensive bioinformatic analysis showing that complex post-transcriptional regulation exists in Lipocalin genes, as suggested by the presence of alternative UTRs with substantial sequence conservation in mammals, alongside a high diversity of transcription start sites and alternative promoters. Strong selective pressure could have operated upon Lipocalins UTRs, leading to an enrichment in particular sequence motifs that limit the choice of secondary structures. Mapping these regulatory features to the expression pattern of early and late diverging Lipocalins suggests that UTRs represent an additional phylogenetic signal, which may help to uncover how functional pleiotropy originated within the Lipocalin family.

摘要

脂质运载蛋白家族是一组具有多种功能的同源蛋白。作为细胞外蛋白,它们可以通过保守的β桶折叠结合小的疏水性配体。脂质运载蛋白的进化历史跨越了许多不同的分类群,甚至在脊索动物中也表现出很大的差异。这种可变性也存在于它们异质的组织表达模式中。尽管之前已经描述了少数启动子区域,但关于脂质运载蛋白基因表达中 UTR 调节作用的研究还很少。在这里,我们报告了一项全面的生物信息学分析,表明脂质运载蛋白基因存在复杂的转录后调控,这是由哺乳动物中具有大量序列保守的替代 UTR 以及转录起始位点和替代启动子的高度多样性所提示的。选择压力可能在脂质运载蛋白的 UTR 上起作用,导致特定序列基序的富集,从而限制了二级结构的选择。将这些调节特征映射到早期和晚期分化的脂质运载蛋白的表达模式上表明,UTR 代表了一个额外的系统发育信号,这可能有助于揭示脂质运载蛋白家族中功能多效性是如何起源的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f9c4/6402760/e4f83d6c3928/pone.0213206.g001.jpg

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