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CAGI experiments: Modeling sequence variant impact on gene splicing using predictions from computational tools

机译:CAGI实验:使用计算工具预测的基因剪接序列变异影响

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Abstract Improving predictions of phenotypic consequences for genomic variants is part of ongoing efforts in the scientific community to gain meaningful insights into genomic function. Within the framework of the critical assessment of genome interpretation experiments, we participated in the Vex‐seq challenge, which required predicting the change in the percent spliced in measure (ΔΨ) for 58 exons caused by more than 1,000 genomic variants. Experimentally determined through the Vex‐seq assay, the Ψ quantifies the fraction of reads that include an exon of interest. Predicting the change in Ψ associated with specific genomic variants implies determining the sequence changes relevant for splicing regulators, such as splicing enhancers and silencers. Here we took advantage of two computational tools, SplicePort and SPANR, that incorporate relevant sequence features in their models of splice sites and exon‐inclusion level, respectively. Specifically, we used the SplicePort and SPANR outputs to build mathematical models of the experimental data obtained for the variants in the training set, which we then used to predict the ΔΨ associated with the mutations in the test set. We show that the sequence changes captured by these computational tools provide a reasonable foundation for modeling the impact on splicing associated with genomic variants.
机译:摘要提高基因组变体表型后果的预测是科学界持续努力的一部分,以获得有意义的洞察力功能。在基因组解释实验的关键评估的框架内,我们参与了VEX-SEQ挑战,这需要预测由1,000多种基因组变体引起的58个外显子的测量(ΔΣ)的百分比变化。通过VEX-SEQ测定进行实验确定,ψ量化包括外显子的读数的分数。预测与特定基因组变体相关的ψ的变化意味着确定对剪接调节器相关的序列变化,例如拼接增强剂和消音器。在这里,我们利用了两个计算工具,SPLICEPORT和SPANR,其分别在其拼接站点和外显纳层的模型中结合了相关的序列特征。具体地,我们使用了SplicePort和SPANR输出来构建用于训练集中的变体获得的实验数据的数学模型,然后我们用于预测与测试集中的突变相关的ΔΣ。我们表明,这些计算工具捕获的序列变化为建模对与基因组变体相关的剪接的影响提供了合理的基础。

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