Complementarity of two proteomic data analysis tools in the identification of drug-metabolising enzymes and transporters in human liver†

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2023-11-13 DOI:10.1039/D3MO00144J
Areti-Maria Vasilogianni, Sarah Alrubia, Eman El-Khateeb, Zubida M. Al-Majdoub, Narciso Couto, Brahim Achour, Amin Rostami-Hodjegan and Jill Barber
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Abstract

Several software packages are available for the analysis of proteomic LC-MS/MS data, including commercial (e.g. Mascot/Progenesis LC-MS) and open access software (e.g. MaxQuant). In this study, Progenesis and MaxQuant were used to analyse the same data set from human liver microsomes (n = 23). Comparison focussed on the total number of peptides and proteins identified by the two packages. For the peptides exclusively identified by each software package, distribution of peptide length, hydrophobicity, molecular weight, isoelectric point and score were compared. Using standard cut-off peptide scores, we found an average of only 65% overlap in detected peptides, with surprisingly little consistency in the characteristics of peptides exclusively detected by each package. Generally, MaxQuant detected more peptides than Progenesis, and the additional peptides were longer and had relatively lower scores. Progenesis-specific peptides tended to be more hydrophilic and basic relative to peptides detected only by MaxQuant. At the protein level, we focussed on drug-metabolising enzymes (DMEs) and transporters, by comparing the number of unique peptides detected by the two packages for these specific proteins of interest, and their abundance. The abundance of DMEs and SLC transporters showed good correlation between the two software tools, but ABC showed less consistency. In conclusion, in order to maximise the use of MS datasets, we recommend processing with more than one software package. Together, Progenesis and MaxQuant provided excellent coverage, with a core of common peptides identified in a very robust way.

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两种蛋白质组数据分析工具在鉴定人类肝脏中药物代谢酶和转运体方面的互补性†。
有几种软件包可用于分析蛋白质组 LC-MS/MS 数据,包括商业软件(如 Mascot/Progenesis LC-MS)和开放软件(如 MaxQuant)。在本研究中,Progenesis 和 MaxQuant 被用于分析来自人类肝脏微粒体(n = 23)的相同数据集。比较的重点是两个软件包鉴定出的肽段和蛋白质的总数。对于每个软件包完全鉴定出的肽段,比较了肽段长度、疏水性、分子量、等电点和得分的分布情况。使用标准的肽段截断分数,我们发现检测到的肽段平均只有 65% 的重叠,而且令人惊讶的是,每个软件包专门检测到的肽段的特征几乎不一致。一般来说,MaxQuant 检测到的肽比 Progenesis 检测到的肽要多,而且额外检测到的肽更长,得分也相对较低。与仅由 MaxQuant 检测到的肽段相比,Progenesis 特有的肽段往往更具亲水性和碱性。在蛋白质层面,我们重点研究了药物代谢酶(DMEs)和转运体,比较了两种软件包为这些特定蛋白质检测到的独特肽段数量及其丰度。DMEs 和 SLC 转运体的丰度在两个软件工具之间显示出良好的相关性,但 ABC 的一致性较差。总之,为了最大限度地利用 MS 数据集,我们建议使用一个以上的软件包进行处理。Progenesis 和 MaxQuant 共同提供了出色的覆盖范围,以非常稳健的方式鉴定出了常见肽段的核心。
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CiteScore
7.20
自引率
4.30%
发文量
567
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