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Evaluation of empirical rule of linearly correlated peptide selection (ERLPS) for proteotypic peptide-based quantitative proteomics

机译:评估线性相关肽选择(ERLPS)基于蛋白肽的定量蛋白质组学的经验规则

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摘要

Precise protein quantification is essential in comparative proteomics. Currently, quantification bias is inevitable when using proteotypic peptide-based quantitative proteomics strategy for the differences in peptides measurability. To improve quantification accuracy, we proposed an "empirical rule for linearly correlated peptide selection (ERLPS)" in quantitative proteomics in our previous work. However, a systematic evaluation on general application of ERLPS in quantitative proteomics under diverse experimental conditions needs to be conducted. In this study, the practice workflow of ERLPS was explicitly illustrated; different experimental variables, such as, different MS systems, sample complexities, sample preparations, elution gradients, matrix effects, loading amounts, and other factors were comprehensively investigated to evaluate the applicability, reproducibility, and transferability of ERPLS. The results demonstrated that ERLPS was highly reproducible and transferable within appropriate loading amounts and linearly correlated response peptides should be selected for each specific experiment. ERLPS was used to proteome samples from yeast to mouse and human, and in quantitative methods from label-free to O18/O16-labeled and SILAC analysis, and enabled accurate measurements for all proteotypic peptide-based quantitative proteomics over a large dynamic range.
机译:精确的蛋白质定量在比较蛋白质组学中至关重要。当前,当使用基于蛋白质型肽的定量蛋白质组学策略来评估肽的可测量性差异时,定量偏差是不可避免的。为了提高定量准确性,我们在先前的工作中在定量蛋白质组学中提出了“线性相关肽选择(ERLPS)的经验规则”。然而,需要在各种实验条件下对ERLPS在定量蛋白质组学中的普遍应用进行系统评价。在这项研究中,ERPPS的实践工作流程得到了明确说明。对不同的实验变量,例如不同的质谱系统,样品的复杂性,样品的制备,洗脱梯度,基质效应,上样量和其他因素进行了综合研究,以评估ERPLS的适用性,可重复性和可转移性。结果表明,ERLPS在适当的上样量内具有很高的重现性和可转移性,应为每个具体实验选择线性相关的响应肽。 ERLPS用于从酵母到小鼠和人的蛋白质组样品,并用于从无标记到O18 / O16标记和SILAC分析的定量方法,并能在大动态范围内对所有基于蛋白质型肽的定量蛋白质组学进行精确测量。

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