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Novel Bisubstrate Inhibitors for Protein N-Terminal Acetyltransferase D

J Med Chem. 2021-06; 
Youchao Deng, Sunbin Deng, Yi-Hsun Ho, Sarah M Gardner, Zhi Huang, Ronen Marmorstein, Rong Huang
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Catalog Peptides  we applied an orthogonal radioactive assay to directly monitor the production of acetylated peptide under a similar condition with both AcCoA and H4–19 peptide substrate (SGRGKGGKGLGKGGAKRHR-COOH; GenScript) at their 4xKm values as radioactive assay is generally more sensitive Get A Quote

摘要

Protein N-terminal acetyltransferase D (NatD, NAA40) that specifically acetylates the alpha-N-terminus of histone H4 and H2A has been implicated in various diseases, but no inhibitor has been reported for this important enzyme. Based on the acetyl transfer mechanism of NatD, we designed and prepared a series of highly potent NatD bisubstrate inhibitors by covalently linking coenzyme A to different peptide substrates via an acetyl or propionyl spacer. The most potent bisubstrate inhibitor displayed an apparent value of 1.0 nM. Biochemical studies indicated that bisubstrate inhibitors are competitive to the peptide substrate and noncompetitive to the cofactor, suggesting that NatD undergoes an ordered Bi-Bi mech... More

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