作为元蛋白质组复杂性衡量标准的谱熵。

IF 3.4 4区 生物学 Q2 BIOCHEMICAL RESEARCH METHODS Proteomics Pub Date : 2024-05-25 DOI:10.1002/pmic.202300570
Haonan Duan, Zhibin Ning, Ailing Zhang, Daniel Figeys
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引用次数: 0

摘要

微生物组基因组图谱的多样性和复杂性并不总是反映在其蛋白质组图谱上。尽管蛋白质组具有预期的多样性,但观察到的微生物组样本的复杂性往往低于预期。造成这种差异的主要因素有两个:质谱检测灵敏度的局限性和元蛋白组学鉴定所面临的生物信息学挑战。本研究引入了一种新方法,直接在全质谱(MS1)水平上评估样品的复杂性,而不是依赖于肽的鉴定。在相同的质谱条件下进行分析时,与单一物种样本相比,微生物组样本显示出明显更高的复杂性,光谱熵和候选肽熵都证明了这一点。这项研究为蛋白质组学中微生物组的复杂性提供了确凿证据,显示了生物信息学工作流程的优化潜力。
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Spectral entropy as a measure of the metaproteome complexity

The diversity and complexity of the microbiome's genomic landscape are not always mirrored in its proteomic profile. Despite the anticipated proteomic diversity, observed complexities of microbiome samples are often lower than expected. Two main factors contribute to this discrepancy: limitations in mass spectrometry's detection sensitivity and bioinformatics challenges in metaproteomics identification. This study introduces a novel approach to evaluating sample complexity directly at the full mass spectrum (MS1) level rather than relying on peptide identifications. When analyzing under identical mass spectrometry conditions, microbiome samples displayed significantly higher complexity, as evidenced by the spectral entropy and peptide candidate entropy, compared to single-species samples. The research provides solid evidence for the complexity of microbiome in proteomics indicating the optimization potential of the bioinformatics workflow.

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来源期刊
Proteomics
Proteomics 生物-生化研究方法
CiteScore
6.30
自引率
5.90%
发文量
193
审稿时长
3 months
期刊介绍: PROTEOMICS is the premier international source for information on all aspects of applications and technologies, including software, in proteomics and other "omics". The journal includes but is not limited to proteomics, genomics, transcriptomics, metabolomics and lipidomics, and systems biology approaches. Papers describing novel applications of proteomics and integration of multi-omics data and approaches are especially welcome.
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