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Identification of diverse target RNAs that are functionally regulated by human Pumilio proteins

机译:鉴定人类Pumilio蛋白在功能调节的不同靶RNA

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Human Pumilio proteins, PUM1 and PUM2, are sequence specific RNA-binding proteins that regulate protein expression. We used RNA-seq, rigorous statistical testing and an experimentally derived fold change cut-off to identify nearly 1000 target RNAs-including mRNAs and non-coding RNAs-that are functionally regulated by PUMs. Bioinformatic analysis defined a PUM Response Element (PRE) that was significantly enriched in transcripts that increased in abundance and matches the PUM RNA-binding consensus. We created a computational model that incorporates PRE position and frequency within an RNA relative to the magnitude of regulation. The model reveals significant correlation of PUM regulation with PREs in 3' untranslated regions (UTRs), coding sequences and non-coding RNAs, but not 5' UTRs. To define direct, high confidence PUM targets, we cross-referenced PUM-regulated RNAs with all PRE-containing RNAs and experimentally defined PUM-bound RNAs. The results define nearly 300 direct targets that include both PUM-repressed and, surprisingly, PUM-activated target RNAs. Annotation enrichment analysis reveal that PUMs regulate genes from multiple signaling pathways and developmental and neurological processes. Moreover, PUM target mRNAs impinge on human disease genes linked to cancer, neurological disorders and cardiovascular disease. These discoveries pave the way for determining how the PUM-dependent regulatory network impacts biological functions and disease states.
机译:人的Pumilio蛋白,Pum1和Pum2是序列特异性RNA结合蛋白,其调节蛋白质表达。我们使用RNA-SEQ,严格的统计测试和实验衍生的折叠变化切断,以识别近1000个靶RNA - 包括MRNA和非编码RNA--在功能上由PUMS调节。生物信息分析定义了显着富集在丰度的转录物中的乳胶反应元素(前),并与PUM RNA结合共识相匹配。我们创建了一种计算模型,其在RNA内相对于调节幅度包含预先定位和频率。该模型揭示了PUM调节与3'未翻译区域(UTRS),编码序列和非编码RNA的显着相关性,但不是5'UTRS。为了定义直接,高置信化妆品靶标,我们用所有预先含的RNA和实验确定的PUM结合的RNA交叉引用的PUM调节的RNA。结果定义了近300个直接靶标,包括PUM抑制,令人惊讶的是,PUM活化的靶RNA。注释富集分析表明,PUMS调节来自多个信号通路和发育和神经过程的基因。此外,PUM靶MRNA撞击与癌症,神经疾病和心血管疾病相关的人类疾病基因。这些发现铺平了确定Pum依赖监管网络如何影响生物功能和疾病状态的方法。

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