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TAPAS: tools to assist the targeted protein quantification of human alternative splice variants

机译:TAPAS:辅助人类替代剪接变体靶向蛋白质定量的工具

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Motivation: In proteomes of higher eukaryotes, many alternative splice variants can only be detected by their shared peptides. This makes it highly challenging to use peptide-centric mass spectrometry to distinguish and to quantify protein isoforms resulting from alternative splicing events.Results: We have developed two complementary algorithms based on linear mathematical models to efficiently compute a minimal set of shared and unique peptides needed to quantify a set of isoforms and splice variants. Further, we developed a statistical method to estimate the splice variant abundances based on stable isotope labeled peptide quantities. The algorithms and databases are integrated in a web-based tool, and we have experimentally tested the limits of our quantification method using spiked proteins and cell extracts
机译:动机:在高等真核生物的蛋白质组中,许多替代剪接变体只能通过它们共享的肽来检测。结果:我们已经开发了两个基于线性数学模型的互补算法,可以有效地计算所需的最小共享和独特肽组,这对使用交替剪接事件产生的蛋白质同工型进行区分和定量具有很高的挑战性。量化一组同工型和剪接变体。此外,我们开发了一种统计方法,可根据稳定的同位素标记的肽数量来估算剪接变体的丰度。算法和数据库集成在基于Web的工具中,我们已经使用加标蛋白质和细胞提取物实验性地测试了定量方法的局限性

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