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摘要:
Drug target discovery is the basis of drug screening.It elucidates the cause of disease and the mechanism of drug action,which is the essential of drug innovation.Target discovery performed in biological sys-tems is complicated as proteins are in low abundance and endogenous compounds may interfere with drug binding.Therefore,methods to track drug-target interactions in biological matrices are urgently required.In this work,a Fe3O4 nanoparticle-based approach was developed for drug-target screening in biofluids.A known ligand-protein complex was selected as a principle-to-proof example to validate the feasibility.After incubation in cell lysates,ligand-modified Fe3O4 nanoparticles bound to the target protein and formed complexes that were separated from the lysates by a magnet for further analysis.The large surface-to-volume ratio of the nanoparticles provides more active sites for the modification of chemical drugs.It enhances the opportunity for ligand-protein interactions,which is beneficial for capturing target proteins,especially for those with low abundance.Additionally,a one-step magnetic separation simplifies the pre-processing of ligand-protein complexes,so it effectively reduces the endogenous interference.Therefore,the present nanoparticle-based approach has the potential to be used for drug target screening in biological systems.
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篇名 Drug target discovery by magnetic nanoparticles coupled mass spectrometry
来源期刊 药物分析学报(英文版) 学科
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年,卷(期) 2021,(1) 所属期刊栏目 Short Communication
研究方向 页码范围 122-127
页数 6页 分类号
字数 语种 英文
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引文网络交叉学科
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期刊影响力
药物分析学报(英文)
双月刊
2095-1779
61-1484/R
大16开
西安市雁塔西路76号
1985
eng
出版文献量(篇)
639
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0
总被引数(次)
912
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