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Poly(A) code analyses reveal key determinants for tissue-specific mRNA alternative polyadenylation

机译:Poly(A)代码分析揭示组织特异性mRNA替代性聚腺苷酸化的关键决定因素

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摘要

mRNA alternative polyadenylation (APA) is a critical mechanism for post-transcriptional gene regulation and is often regulated in a tissue-and/or developmental stage-specific manner. An ultimate goal for the APA field has been to be able to computationally predict APA profiles under different physiological or pathological conditions. As a first step toward this goal, we have assembled a poly(A) code for predicting tissue-specific poly(A) sites (PASs). Based on a compendium of over 600 features that have known or potential roles in PAS selection, we have generated and refined a machine-learning algorithm using multiple high-throughput sequencing-based data sets of tissue-specific and constitutive PASs. This code can predict tissue-specific PASs with >85% accuracy. Importantly, by analyzing the prediction performance based on different RNA features, we found that PAS context, including the distance between alternative PASs and the relative position of a PAS within the gene, is a key feature for determining the susceptibility of a PAS to tissue-specific regulation. Our poly(A) code provides a useful tool for not only predicting tissue-specific APA regulation, but also for studying its underlying molecular mechanisms.
机译:mRNA替代性聚腺苷酸化(APA)是转录后基因调控的关键机制,通常以组织和/或发育阶段特异性的方式进行调控。 APA领域的最终目标是能够通过计算预测不同生理或病理条件下的APA分布。作为朝着这个目标迈出的第一步,我们已经组装了poly(A)代码,用于预测组织特异性的poly(A)位点(PAS)。基于在PAS选择中具有已知或潜在作用的600多种功能的概述,我们使用组织特异性和组成性PAS的多个基于高通量测序的数据集生成并完善了机器学习算法。此代码可以预测组织特定的PAS,准确率> 85%。重要的是,通过分析基于不同RNA特征的预测性能,我们发现PAS上下文(包括替代PAS之间的距离和基因内PAS的相对位置)是确定PAS对组织敏感性的关键特征-具体规定。我们的poly(A)代码不仅为预测组织特异性APA调控提供了有用的工具,而且还可以用于研究其潜在的分子机制。

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