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MicroRNAs and Cancer—The Search Begins!

机译:MicroRNA和癌症-搜索开始!

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摘要

For almost three decades, cancer was thought to result from changes in the structure and/or expression of protein coding genes. The discovery of thousands of genes that produce noncoding RNA (ncRNA) transcripts in the past few years suggested that the molecular biology of cancer is much more complex. MicroRNAs (miRNAs), an important group of ncRNAs, have recently been associated with tumorigenesis by acting either as tumor suppressors or oncogenes. Experimental prediction of miRNA genes is a slow process, because of the difficulties of cloning ncRNAs. Complementary to experimental approaches, a number of computational tools trained to recognize features of the biogenesis of miRNAs have significantly aided in the prediction of new miRNA candidates. By narrowing down the search space, computational approaches provide valuable clues as to which are the dominant features that characterize these regulatory units and which genes are their most likely targets. Moreover, through the use of high-throughput expression profiling methods, many molecular signatures of miRNA deregulation in human tumors have emerged. In this review, we present an overview of existing computational methods for identifying miRNA genes and assessing their expression levels, and analyze the contribution of such tools toward illuminating the role of miRNAs in cancer.
机译:近三十年来,人们一直认为癌症是由蛋白质编码基因的结构和/或表达的变化导致的。在过去几年中发现了数千种产生非编码RNA(ncRNA)转录本的基因,这表明癌症的分子生物学要复杂得多。 MicroRNA(miRNA)是重要的ncRNA组,最近通过充当肿瘤抑制因子或致癌基因而与肿瘤发生相关。由于克隆ncRNA的困难,miRNA基因的实验预测是一个缓慢的过程。作为实验方法的补充,许多训练有素的计算机工具可以识别miRNA的生物发生特征,从而大大有助于预测新的miRNA候选物。通过缩小搜索空间,计算方法可提供有价值的线索,以了解哪些是表征这些调控单元的主要特征,哪些基因是其最可能的靶标。此外,通过使用高通量表达谱分析方法,已经出现了人类肿瘤中许多miRNA失调的分子标记。在这篇综述中,我们概述了用于识别miRNA基因并评估其表达水平的现有计算方法,并分析了此类工具对阐明miRNA在癌症中的作用的贡献。

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