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Prediction of viral microRNA precursors based on human microRNA precursor sequence and structural features

机译:基于人microRNA前体序列和结构特征的病毒microRNA前体预测

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MicroRNAs (small ~22 nucleotide long non-coding endogenous RNAs) have recently attracted immense attention as critical regulators of gene expression in multi-cellular eukaryotes, especially in humans. Recent studies have proved that viruses also express microRNAs, which are thought to contribute to the intricate mechanisms of host-pathogen interactions. Computational predictions have greatly accelerated the discovery of microRNAs. However, most of these widely used tools are dependent on structural features and sequence conservation which limits their use in discovering novel virus expressed microRNAs and non-conserved eukaryotic microRNAs. In this work an efficient prediction method is developed based on the hypothesis that sequence and structure features which discriminate between host microRNA precursor hairpins and pseudo microRNAs are shared by viral microRNA as they depend on host machinery for the processing of microRNA precursors. The proposed method has been found to be more efficient than recently reported ab-initio methods for predicting viral microRNAs and microRNAs expressed by mammals.
机译:作为多细胞真核生物(尤其是人类)中基因表达的关键调节因子,MicroRNA(约22个核苷酸长的非编码内源性小RNA)最近引起了极大的关注。最近的研究证明病毒还表达microRNA,据认为它们有助于宿主与病原体相互作用的复杂机制。计算预测大大加快了microRNA的发现。但是,大多数这些广泛使用的工具取决于结构特征和序列保守性,这限制了它们在发现新型病毒表达的microRNA和非保守的真核microRNA中的用途。在这项工作中,基于以下假设开发了一种有效的预测方法,该假设是区分宿主微RNA前体发夹和假微RNA的序列和结构特征被病毒微RNA共享,因为它们依赖于宿主设备来处理微RNA前体。已经发现提出的方法比最近报道的从头开始的方法更有效地预测哺乳动物表达的病毒微小RNA和微小RNA。

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