Chemoproteomic mapping of the glycolytic targetome in cancer cells

糖酵解 生物 生物化学 细胞生物学 计算生物学 计算机科学 新陈代谢
作者
Yang Tian,Ning Wan,Hanqing Zhang,Chang Shao,Ming Ding,Qiuyu Bao,Hai Hu,Huiyong Sun,Chenguang Liu,Kun Zhou,Shuai Chen,Guangji Wang,Hui Ye,Haiping Hao
出处
期刊:Nature Chemical Biology [Springer Nature]
卷期号:19 (12): 1480-1491 被引量:11
标识
DOI:10.1038/s41589-023-01355-w
摘要

Hyperactivated glycolysis is a metabolic hallmark of most cancer cells. Although sporadic information has revealed that glycolytic metabolites possess nonmetabolic functions as signaling molecules, how these metabolites interact with and functionally regulate their binding targets remains largely elusive. Here, we introduce a target-responsive accessibility profiling (TRAP) approach that measures changes in ligand binding-induced accessibility for target identification by globally labeling reactive proteinaceous lysines. With TRAP, we mapped 913 responsive target candidates and 2,487 interactions for 10 major glycolytic metabolites in a model cancer cell line. The wide targetome depicted by TRAP unveils diverse regulatory modalities of glycolytic metabolites, and these modalities involve direct perturbation of enzymes in carbohydrate metabolism, intervention of an orphan transcriptional protein’s activity and modulation of targetome-level acetylation. These results further our knowledge of how glycolysis orchestrates signaling pathways in cancer cells to support their survival, and inspire exploitation of the glycolytic targetome for cancer therapy. A chemoproteomic approach is developed that examines changes in ligand binding-induced accessibility by globally labeling reactive proteinaceous lysines, revealing the cellular targets of glycolytic intermediates.
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