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A proteogenomic approach to understand splice isoform functions through sequence and expression-based computational modeling

机译:一种蛋白质组学方法可通过基于序列和基于表达的计算建模来了解剪接异构体功能

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摘要

The products of multi-exon genes are a mixture of alternatively spliced isoforms, from which the translated proteins can have similar, different or even opposing functions. It is therefore essential to differentiate and annotate functions for individual isoforms. Computational approaches provide an efficient complement to expensive and time-consuming experimental studies. The input data of these methods range from DNA sequence, to RNA selection pressure, to expressed sequence tags, to full-length complementary DNA, to exon array, to RNA-seq expression, to proteomic data. Notably, RNA-seq technology generates quantitative profiling of transcript expression at the genome scale, with an unprecedented amount of expression data available for developing isoform function prediction methods. Integrative analysis of these data at different molecular levels enables a proteogenomic approach to systematically interrogate isoform functions. Here, we briefly review the state-of-the-art methods according to their input data sources, discuss their advantages and limitations and point out potential ways to improve prediction accuracies.
机译:多外显子基因的产物是交替剪接的同工型的混合物,翻译后的蛋白可具有类似,不同或什至相反的功能。因此,区分和注释单个同工型的功能至关重要。计算方法为昂贵且费时的实验研究提供了有效的补充。这些方法的输入数据包括DNA序列,RNA选择压力,表达序列标签,全长互补DNA,外显子阵列,RNA-seq表达和蛋白质组数据。值得注意的是,RNA-seq技术可在基因组规模上生成转录表达的定量分析图,其空前数量的表达数据可用于开发同工型功能预测方法。对这些数据在不同分子水平的综合分析使蛋白质组学方法可以系统地研究同工型功能。在这里,我们根据输入数据源简要回顾了最新技术,讨论了它们的优点和局限性,并指出了提高预测准确性的潜在方法。

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