m6ATM:利用 Nanopore 长读程 RNA-seq 数据解密 m6A 表转录组的深度学习框架。

IF 6.8 2区 生物学 Q1 BIOCHEMICAL RESEARCH METHODS
Boyi Yu, Genta Nagae, Yutaka Midorikawa, Kenji Tatsuno, Bhaskar Dasgupta, Hiroyuki Aburatani, Hiroki Ueda
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引用次数: 0

摘要

自 20 世纪 70 年代发现以来,N6-甲基腺苷(m6A)是信使 RNA 中最丰富、最广为人知的修饰之一。最近的研究表明,m6A 参与了多种生物过程,如替代剪接和 RNA 降解,在多种疾病中发挥着重要作用。要更好地了解 m6A 的作用,全转录组 m6A 图谱数据必不可少。近年来,牛津纳米孔技术公司(Oxford Nanopore Technology)的直接 RNA 测序(DRS)平台已显示出基于转录本中测量到的电流中断进行 RNA 修饰检测的前景。然而,将电流强度数据解码为修饰图谱仍是一项具有挑战性的任务。在这里,我们介绍了 m6A Transcriptome-wide Mapper (m6ATM),这是一种基于 Python 的新型计算管道,它应用深度神经网络,利用 DRS 数据以单碱基分辨率预测 m6A 位点。m6ATM 模型架构包含一个 WaveNet 编码器和一个双流多实例学习模型,用于从特定目标位点提取特征并描述 m6A 表转录组。在验证方面,m6ATM 在包含不同 m6A 修饰比例的体外转录数据集上的准确率达到了 80% 到 98%,在使用人类细胞系数据进行基准测试时的表现优于其他工具。此外,我们还证明了 m6ATM 在提供可靠的化学计量信息方面的多功能性,并利用它将 PEG10 确定为肝癌细胞中潜在的 m6A 目标转录本。总之,m6ATM 是一种高性能的 m6A 检测工具,我们的研究结果为未来表转录组学研究的发展铺平了道路。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
m6ATM: a deep learning framework for demystifying the m6A epitranscriptome with Nanopore long-read RNA-seq data.

N6-methyladenosine (m6A) is one of the most abundant and well-known modifications in messenger RNAs since its discovery in the 1970s. Recent studies have demonstrated that m6A is involved in various biological processes, such as alternative splicing and RNA degradation, playing an important role in a variety of diseases. To better understand the role of m6A, transcriptome-wide m6A profiling data are indispensable. In recent years, the Oxford Nanopore Technology Direct RNA Sequencing (DRS) platform has shown promise for RNA modification detection based on current disruptions measured in transcripts. However, decoding current intensity data into modification profiles remains a challenging task. Here, we introduce the m6A Transcriptome-wide Mapper (m6ATM), a novel Python-based computational pipeline that applies deep neural networks to predict m6A sites at a single-base resolution using DRS data. The m6ATM model architecture incorporates a WaveNet encoder and a dual-stream multiple-instance learning model to extract features from specific target sites and characterize the m6A epitranscriptome. For validation, m6ATM achieved an accuracy of 80% to 98% across in vitro transcription datasets containing varying m6A modification ratios and outperformed other tools in benchmarking with human cell line data. Moreover, we demonstrated the versatility of m6ATM in providing reliable stoichiometric information and used it to pinpoint PEG10 as a potential m6A target transcript in liver cancer cells. In conclusion, m6ATM is a high-performance m6A detection tool, and our results pave the way for future advancements in epitranscriptomic research.

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来源期刊
Briefings in bioinformatics
Briefings in bioinformatics 生物-生化研究方法
CiteScore
13.20
自引率
13.70%
发文量
549
审稿时长
6 months
期刊介绍: Briefings in Bioinformatics is an international journal serving as a platform for researchers and educators in the life sciences. It also appeals to mathematicians, statisticians, and computer scientists applying their expertise to biological challenges. The journal focuses on reviews tailored for users of databases and analytical tools in contemporary genetics, molecular and systems biology. It stands out by offering practical assistance and guidance to non-specialists in computerized methodologies. Covering a wide range from introductory concepts to specific protocols and analyses, the papers address bacterial, plant, fungal, animal, and human data. The journal's detailed subject areas include genetic studies of phenotypes and genotypes, mapping, DNA sequencing, expression profiling, gene expression studies, microarrays, alignment methods, protein profiles and HMMs, lipids, metabolic and signaling pathways, structure determination and function prediction, phylogenetic studies, and education and training.
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