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不同样品制备方法对自上而下蛋白质组学中蛋白质异构体鉴定的影响。

Influence of different sample preparation approaches on proteoform identification by top-down proteomics.

作者信息

Kaulich Philipp T, Jeong Kyowon, Kohlbacher Oliver, Tholey Andreas

机构信息

Systematic Proteome Research and Bioanalytics, Institute for Experimental Medicine, Christian-Albrechts-Universität zu Kiel, Kiel, Germany.

Applied Bioinformatics, Computer Science Department, University of Tübingen, Tübingen, Germany.

出版信息

Nat Methods. 2024 Dec;21(12):2397-2407. doi: 10.1038/s41592-024-02481-6. Epub 2024 Oct 22.

Abstract

Top-down proteomics using mass spectrometry facilitates the identification of intact proteoforms, that is, all molecular forms of proteins. Multiple past advances have lead to the development of numerous sample preparation workflows. Here we systematically investigated the influence of different sample preparation steps on proteoform and protein identifications, including cell lysis, reduction and alkylation, proteoform enrichment, purification and fractionation. We found that all steps in sample preparation influence the subset of proteoforms identified (for example, their number, confidence, physicochemical properties and artificially generated modifications). The various sample preparation strategies resulted in complementary identifications, substantially increasing the proteome coverage. Overall, we identified 13,975 proteoforms from 2,720 proteins of human Caco-2 cells. The results presented can serve as suggestions for designing and adapting top-down proteomics sample preparation strategies to particular research questions. Moreover, we expect that the sampling bias and modifications identified at the intact protein level will also be useful in improving bottom-up proteomics approaches.

摘要

使用质谱的自上而下蛋白质组学有助于完整蛋白质变体(即蛋白质的所有分子形式)的鉴定。过去的多项进展已促成众多样品制备工作流程的发展。在此,我们系统地研究了不同样品制备步骤对蛋白质变体和蛋白质鉴定的影响,包括细胞裂解、还原和烷基化、蛋白质变体富集、纯化和分级分离。我们发现样品制备中的所有步骤都会影响所鉴定的蛋白质变体子集(例如,它们的数量、可信度、物理化学性质和人为产生的修饰)。各种样品制备策略导致了互补的鉴定结果,大幅提高了蛋白质组覆盖率。总体而言,我们从人Caco-2细胞的2720种蛋白质中鉴定出13975种蛋白质变体。所呈现的结果可为设计和调整自上而下蛋白质组学样品制备策略以适应特定研究问题提供建议。此外,我们预计在完整蛋白质水平上鉴定出的采样偏差和修饰也将有助于改进自下而上的蛋白质组学方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1919/11621018/a4f10d9ff3cc/41592_2024_2481_Fig1_HTML.jpg

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