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Large scale chromosomal mapping of human microRNA structural clusters

机译:人类microRNA结构簇的大规模染色体作图

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MicroRNAs (miRNAs) can group together along the human genome to form stable secondary structures made of several hairpins hosting miRNAs in their stems. The few known examples of such structures are all involved in cancer development. A large scale computational analysis of human chromosomes crossing sequence analysis and deep sequencing data revealed the presence of > 400 structural clusters of miRNAs in the human genome. An a posteriori analysis validates predictions as bona fide miRNAs. A functional analysis of structural clusters position along the chromosomes co-localizes them with genes involved in several key cellular processes like immune systems, sensory systems, signal transduction and development. Immune systems diseases, infectious diseases and neurodegenerative diseases are characterized by genes that are especially well organized around structural clusters of miRNAs. Target genes functional analysis strongly supports a regulatory role of most predicted miRNAs and, notably, a strong involvement of predicted miRNAs in the regulation of cancer pathways. This analysis provides new fundamental insights on the genomic organization of miRNAs in human chromosomes.
机译:MicroRNA(miRNA)可以沿着人类基因组聚集在一起,形成稳定的二级结构,该二级结构由在其茎中托管miRNA的多个发夹组成。这种结构的几个已知例子都参与了癌症的发展。对人类染色体的大规模计算分析,交叉序列分析和深度测序数据表明,人类基因组中存在超过400个miRNA结构簇。后验分析证实了预测为真正的miRNA。对沿着染色体的结构簇位置的功能分析使它们与涉及多个关键细胞过程(如免疫系统,感觉系统,信号转导和发育)的基因共定位。免疫系统疾病,感染性疾病和神经退行性疾病的特征是基因,这些基因在miRNA的结构簇周围特别有条理。靶基因功能分析强烈支持大多数预测的miRNA的调控作用,尤其是预测的miRNA参与癌症通路的调控。该分析为人类染色体中miRNA的基因组组织提供了新的基本见解。

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