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一种增强鼠粪便宏蛋白质组学分类和功能覆盖的集成工作流程。

An integrated workflow for enhanced taxonomic and functional coverage of the mouse fecal metaproteome.

机构信息

Proteome Center Tuebingen, University of Tuebingen, Tuebingen, Germany.

Biomolecular Medicine Section, Division of Systems Medicine, Department of Metabolism, Digestion and Reproduction, Imperial College London, London, UK.

出版信息

Gut Microbes. 2021 Jan-Dec;13(1):1994836. doi: 10.1080/19490976.2021.1994836.

Abstract

Intestinal microbiota plays a key role in shaping host homeostasis by regulating metabolism, immune responses and behavior. Its dysregulation has been associated with metabolic, immune and neuropsychiatric disorders and is accompanied by changes in bacterial metabolic regulation. Although proteomics is well suited for analysis of individual microbes, metaproteomics of fecal samples is challenging due to the physical structure of the sample, presence of contaminating host proteins and coexistence of hundreds of taxa. Furthermore, there is a lack of consensus regarding preparation of fecal samples, as well as downstream bioinformatic analyses following metaproteomics data acquisition. Here we assess sample preparation and data analysis strategies applied to mouse feces in a typical mass spectrometry-based metaproteomic experiment. We show that subtle changes in sample preparation protocols may influence interpretation of biological findings. Two-step database search strategies led to significant underestimation of false positive protein identifications. Unipept software provided the highest sensitivity and specificity in taxonomic annotation of the identified peptides of unknown origin. Comparison of matching metaproteome and metagenome data revealed a positive correlation between protein and gene abundances. Notably, nearly all functional categories of detected protein groups were differentially abundant in the metaproteome compared to what would be expected from the metagenome, highlighting the need to perform metaproteomics when studying complex microbiome samples.

摘要

肠道微生物群通过调节代谢、免疫反应和行为,在塑造宿主内稳态方面发挥着关键作用。其失调与代谢、免疫和神经精神疾病有关,并伴随着细菌代谢调节的变化。尽管蛋白质组学非常适合分析单个微生物,但由于粪便样本的物理结构、宿主蛋白的污染以及数百个分类群的共存,粪便样本的宏蛋白质组学分析具有挑战性。此外,在粪便样本的准备以及宏蛋白质组学数据采集后的下游生物信息学分析方面,缺乏共识。在这里,我们评估了在典型的基于质谱的宏蛋白质组学实验中应用于小鼠粪便的样品制备和数据分析策略。我们表明,样品制备方案的细微变化可能会影响对生物学发现的解释。两步数据库搜索策略导致假阳性蛋白鉴定的显著低估。Unipept 软件在对未知来源的鉴定肽进行分类注释方面提供了最高的灵敏度和特异性。匹配的宏蛋白质组和宏基因组数据的比较表明,蛋白质和基因丰度之间存在正相关。值得注意的是,与从宏基因组中预期的相比,检测到的蛋白组的几乎所有功能类别在宏蛋白质组中都存在差异丰度,这突出了在研究复杂微生物组样本时进行宏蛋白质组学的必要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0a49/8726736/97c1b0ae3f6c/KGMI_A_1994836_F0001_OC.jpg

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