Spike-In Proteome Enhances Data-Independent Acquisition for Thermal Proteome Profiling
文献类型: 外文期刊
第一作者: Wang, Qiqi
作者: Wang, Qiqi;Chen, Qiufen;Lin, Yue;He, Dan;Tan, Chris Soon Heng;Wang, Qiqi;Chen, Qiufen;Lin, Yue;He, Dan;Tan, Chris Soon Heng;Ji, Hongchao;Wang, Qiqi;Chen, Qiufen;Lin, Yue;He, Dan;Tan, Chris Soon Heng
作者机构:
期刊名称:ANALYTICAL CHEMISTRY ( 影响因子:6.7; 五年影响因子:6.6 )
ISSN: 0003-2700
年卷期: 2024 年 96 卷 49 期
页码:
收录情况: SCI
摘要: Target deconvolution is essential for elucidating the molecular mechanisms, therapeutic efficacy, and off-target toxicity of small-molecule drugs. Thermal proteome profiling (TPP) is a robust and popular method for identifying drug-protein interactions. Nevertheless, classical implementation of TPP using isobaric labeling of peptides is tedious, time-consuming, and costly. This prompts the adoption of a label-free approach with data-independent acquisition (DIA), but with substantial compromise in protein coverage and precision. To address these shortcomings, we improvised a spike-in proteome strategy for DIA with TPP to counteract the reduction in protein quantity following sample heating. Protein coverage, data completeness, and quantification precision are significantly improved as result. Additionally, a calibration algorithm was developed to correct for spike-in effects on fold changes. The integration of DIA-TPP with the matrix-augmented pooling strategy (MAPS) to increase experiment throughput demonstrates performance comparable to that of existing TMT-TPP-MAPS. With this spike-in proteome strategy, we also successfully identified the thermal stabilization of CA13 by dorzolamide hydrochloride as well as GSTZ1 and tyrosyl-DNA phosphodiesterase 1 of opicapone that eluded detection without spike-in proteome.
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