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Computational Detection of Alternative Exon Usage

机译:替代性外显子用法的计算检测

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Background: With the advent of the GeneChip Exon Arrays, it is now possible to extract "exon-level" expression estimates, allowing for detection of alternative splicing events, one of the primary mechanisms of transcript diversity. In the context of 1) a complex trait use case and 2) a human cerebellum vs. heart comparison on previously validated data, we present a transcript-based statistical model and validation framework to allow detection of alternative exon usage (AEU) between different groups. To illustrate the approach, we detect and confirm differences in exon usage in the two of the most widely studied mouse genetic models (the C57BL/6J and DBA/2J inbred strains) and in a human dataset. Results: We developed a computational framework that consists of probe level annotation mapping and statistical modelling to detect putative AEU events, as well as visualization and alignment with known splice events. We show a dramatic improvement (~25 fold) in the ability to detect these events using the appropriate annotation and statistical model which is actually specified at the transcript level, as compared with the transcript cluster/gene level annotation used on the array. An additional component of this workflow is a probe index that allows ranking AEU candidates for validation and can aid in identification of false positives due to single nucleotide polymorphisms. Discussion: Our work highlights the importance of concordance between the functional unit interrogated (e.g., gene, transcripts) and the entity (e.g., exon, probeset) within the statistical model. The framework we present is broadly applicable to other platforms (including RNAseq).
机译:背景:随着GeneChip外显子阵列的出现,现在有可能提取“外显子级”表达估计,从而允许检测其他剪接事件,这是转录本多样性的主要机制之一。在1)复杂性状使用案例和2)在先前验证的数据上进行人类小脑与心脏比较的情况下,我们提出了一个基于转录本的统计模型和验证框架,以允许检测不同组之间的替代性外显子使用(AEU) 。为了说明这种方法,我们在两个研究最广泛的小鼠遗传模型(C57BL / 6J和DBA / 2J自交系)和人类数据集中检测并确认外显子用法的差异。结果:我们开发了一个计算框架,该框架由探针级别注释映射和统计模型组成,以检测假定的AEU事件,以及可视化和与已知剪接事件的比对。与阵列上使用的转录簇/基因水平注释相比,我们使用在转录本水平实际指定的适当注释和统计模型,在检测这些事件的能力方面显示出显着的提高(〜25倍)。此工作流程的另一个组成部分是探针索引,该探针索引可对AEU候选者进行排名以进行验证,并且可以帮助识别由于单核苷酸多态性而导致的假阳性。讨论:我们的工作强调了统计模型中被询问的功能单元(例如基因,转录本)与实体(例如外显子,探针集)之间保持一致的重要性。我们提出的框架广泛适用于其他平台(包括RNAseq)。

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