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分析人类上游开放阅读框及其对基因表达的影响。

Analysis of human upstream open reading frames and impact on gene expression.

机构信息

Department of Medical Genetics, School of Basic Medical Sciences, Southern Medical University, Guangzhou, China.

出版信息

Hum Genet. 2015 Jun;134(6):605-12. doi: 10.1007/s00439-015-1544-7. Epub 2015 Mar 24.

DOI:10.1007/s00439-015-1544-7
PMID:25800702
Abstract

The upstream open reading frame (uORF) is a post-transcriptional regulatory element in the 5' untranslated region (5'UTR), which modulates the translation levels of main open reading frame (mORF). Earlier studies showed that disturbed uORF-mediated translation control can result in drastic changes in translation levels of mORF, leading to genetic disorders. To date, there has been no systematic investigation into the relationship between variations in patients and uORF status. Here, taking the advantage of several datasets, including gene ontology (GO) annotations and sequence feature analysis, we have examined uORF impacts in human transcripts. GO annotations indicate that uORF-containing genes are enriched in certain features such as oncogenes and transcription factors. Sequence feature analysis reveals that uORF is a factor for determination of the translation initiation site (TIS) in human transcripts. We show that genes with uORFs have lower protein expression levels than genes without uORFs in multiple human tissues. Moreover, by examining three disease variation databases, we identified uORF-altering mutations from a total of 3,740,225 variations, which are highly suspected to be associated with changed levels of gene expression. For an experimental validation, we found four mutations with significant effects on protein expression but with only modest changes in transcription levels. These findings will provide researchers on related diseases with new insights into the importance of known mutations.

摘要

上游开放阅读框 (uORF) 是 5' 非翻译区 (5'UTR) 中的一种转录后调控元件,可调节主要开放阅读框 (mORF) 的翻译水平。早期研究表明,uORF 介导的翻译调控失调可导致 mORF 翻译水平的剧烈变化,从而导致遗传疾病。迄今为止,尚未对患者变异与 uORF 状态之间的关系进行系统研究。在这里,我们利用包括基因本体 (GO) 注释和序列特征分析在内的多个数据集,研究了 uORF 在人类转录本中的作用。GO 注释表明,含有 uORF 的基因富集于某些特征,如癌基因和转录因子。序列特征分析表明,uORF 是决定人类转录本翻译起始位点 (TIS) 的因素。我们表明,在多个人类组织中,含有 uORF 的基因的蛋白质表达水平低于没有 uORF 的基因。此外,通过检查三个疾病变异数据库,我们从总共 3740225 个变异中鉴定出了改变 uORF 的突变,这些突变高度怀疑与基因表达水平的变化有关。为了进行实验验证,我们发现了四个对蛋白质表达有显著影响但转录水平仅有适度变化的突变。这些发现将为相关疾病的研究人员提供新的见解,了解已知突变的重要性。

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