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HOXD-AS1是一种在HOXD基因簇中编码的新型长链非编码RNA,是通过对非编码转录组进行综合分析揭示的神经母细胞瘤进展的标志物。

HOXD-AS1 is a novel lncRNA encoded in HOXD cluster and a marker of neuroblastoma progression revealed via integrative analysis of noncoding transcriptome.

作者信息

Yarmishyn Aliaksandr A, Batagov Arsen O, Tan Jovina Z, Sundaram Gopinath M, Sampath Prabha, Kuznetsov Vladimir A, Kurochkin Igor V

出版信息

BMC Genomics. 2014;15 Suppl 9(Suppl 9):S7. doi: 10.1186/1471-2164-15-S9-S7. Epub 2014 Dec 8.

Abstract

BACKGROUND

Long noncoding RNAs (lncRNAs) constitute a major, but poorly characterized part of human transcriptome. Recent evidence indicates that many lncRNAs are involved in cancer and can be used as predictive and prognostic biomarkers. Significant fraction of lncRNAs is represented on widely used microarray platforms, however they have usually been ignored in cancer studies.

RESULTS

We developed a computational pipeline to annotate lncRNAs on popular Affymetrix U133 microarrays, creating a resource allowing measurement of expression of 1581 lncRNAs. This resource can be utilized to interrogate existing microarray datasets for various lncRNA studies. We found that these lncRNAs fall into three distinct classes according to their statistical distribution by length. Remarkably, these three classes of lncRNAs were co-localized with protein coding genes exhibiting distinct gene ontology groups. This annotation was applied to microarray analysis which identified a 159 lncRNA signature that discriminates between localized and metastatic stages of neuroblastoma. Analysis of an independent patient cohort revealed that this signature differentiates also relapsing from non-relapsing primary tumors. This is the first example of the signature developed via the analysis of expression of lncRNAs solely. One of these lncRNAs, termed HOXD-AS1, is encoded in HOXD cluster. HOXD-AS1 is evolutionary conserved among hominids and has all bona fide features of a gene. Studying retinoid acid (RA) response of SH-SY5Y cell line, a model of human metastatic neuroblastoma, we found that HOXD-AS1 is a subject to morphogenic regulation, is activated by PI3K/Akt pathway and itself is involved in control of RA-induced cell differentiation. Knock-down experiments revealed that HOXD-AS1 controls expression levels of clinically significant protein-coding genes involved in angiogenesis and inflammation, the hallmarks of metastatic cancer.

CONCLUSIONS

Our findings greatly extend the number of noncoding RNAs functionally implicated in tumor development and patient treatment and highlight their role as potential prognostic biomarkers of neuroblastomas.

摘要

背景

长链非编码RNA(lncRNAs)构成了人类转录组的主要部分,但特征描述较少。最近的证据表明,许多lncRNAs与癌症相关,可作为预测和预后生物标志物。lncRNAs的很大一部分在广泛使用的微阵列平台上有体现,然而在癌症研究中它们通常被忽视。

结果

我们开发了一种计算流程,用于注释常用的Affymetrix U133微阵列上的lncRNAs,创建了一个可用于测量1581种lncRNAs表达的资源。该资源可用于查询现有的微阵列数据集以进行各种lncRNA研究。我们发现,这些lncRNAs根据其长度的统计分布可分为三个不同的类别。值得注意的是,这三类lncRNAs与表现出不同基因本体组的蛋白质编码基因共定位。这种注释应用于微阵列分析,确定了一个可区分神经母细胞瘤局部和转移阶段的159个lncRNA特征。对一个独立患者队列的分析表明,该特征也能区分复发性和非复发性原发性肿瘤。这是通过仅分析lncRNAs表达而开发的特征的首个实例。这些lncRNAs之一,称为HOXD-AS1,在HOXD簇中编码。HOXD-AS1在人科动物中具有进化保守性,具有基因的所有真实特征。研究人类转移性神经母细胞瘤模型SH-SY5Y细胞系的视黄酸(RA)反应时,我们发现HOXD-AS1受形态发生调控,被PI3K/Akt途径激活,且自身参与RA诱导的细胞分化控制。敲低实验表明,HOXD-AS1控制参与血管生成和炎症的临床重要蛋白质编码基因的表达水平,而血管生成和炎症是转移性癌症的标志。

结论

我们的发现极大地扩展了在肿瘤发生发展和患者治疗中具有功能意义的非编码RNA的数量,并突出了它们作为神经母细胞瘤潜在预后生物标志物的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b063/4290621/d3e1ca556ed1/1471-2164-15-S9-S7-1.jpg

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