化学
质谱法
串联质谱法
结合
共价键
肽
色谱法
组合化学
有机化学
生物化学
数学
数学分析
作者
Peiyuan Zhang,Xiyun Ye,John Wang,Hannah T. Baddock,Zena D. Jensvold,Ian T. Foe,Andrei Loas,Dan Eaton,Qi Hao,Aaron H. Nile,Bradley L. Pentelute
摘要
Covalent peptide binders have found applications as activity-based probes and as irreversible therapeutic inhibitors. Currently, there is no rapid, label-free, and tunable affinity selection platform to enrich covalent reactive peptide binders from synthetic libraries. We address this challenge by developing a reversibly reactive affinity selection platform termed ReAct-ASMS enabled by tandem high-resolution mass spectrometry (MS/MS) to identify covalent peptide binders to native protein targets. It uses mixed disulfide-containing peptides to build reversible peptide-protein conjugates that can enrich for covalent variants, which can be sequenced by MS/MS after reduction. Using this platform, we identified covalent peptide binders against two oncoproteins, human papillomavirus 16 early protein 6 (HPV16 E6) and peptidyl-prolyl
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