| Literature DB >> 33861519 |
Emmanuel K Toroitich1, Anthony M Ciancone1, Heung Sik Hahm1, Skylar M Brodowski1, Adam H Libby1,2, Ku-Lung Hsu1,3,4,2.
Abstract
Sulfonyl-triazoles have emerged as a new reactive group for covalent modification of tyrosine sites on proteins through sulfur-triazole exchange (SuTEx) chemistry. The extent to which this sulfur electrophile can be tuned for developing ligands with cellular activity remains largely underexplored. Here, we performed fragment-based ligand discovery in live cells to identify SuTEx compounds capable of liganding tyrosine sites on diverse protein targets. We verified our quantitative chemical proteomic findings by demonstrating concentration-dependent activity of SuTEx ligands, but not inactive counterparts, against recombinant protein targets directly in live cells. Our structure-activity relationship studies identified the SuTEx ligand HHS-0701 as a cell-active inhibitor capable of blocking prostaglandin reductase 2 (PTGR2) biochemical activity.Entities:
Keywords: Activity-based protein profiling; SuFEx; SuTEx; chemical proteomics; fragment-based ligand discovery
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Year: 2021 PMID: 33861519 PMCID: PMC8206015 DOI: 10.1002/cbic.202000879
Source DB: PubMed Journal: Chembiochem ISSN: 1439-4227 Impact factor: 3.461