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Literature DB >> 30637990

Bisubstrate inhibitors to target histone acetyltransferase 1.

Liza Ngo¹, Tyler Brown¹, Yujun G Zheng¹.

Abstract

Developing selective enzyme inhibitors allows for the expansion of molecular toolboxes to investigate functions and activities of target enzymes. The histone acetyltransferase 1 (HAT1) is among the first histone acetyltransferase (HAT) enzymes that were discovered in the mid-1990s; however, it remains one of the poorly studied enzymes in comparison with the other HATs. Although HAT1 has been linked to various disease states, no inhibitors have been reported to target HAT1. Here, we designed a set of peptide-CoA conjugates as bisubstrate inhibitors of HAT1 with submicromolar potency. In particular, the bisubstrate inhibitor H4K12CoA exhibited a low Ki value of 1.1 nM for HAT1. In addition, H4K12CoA was shown to be a competitive inhibitor with respect to both AcCoA and H4 peptide, suggesting a unique kinetic mechanism of HAT1 catalysis. Creating these submicromolar inhibitors offers mechanistic tools to better understand how HAT1 recognizes substrates and cofactors, as well as provides chemical leads to further develop therapeutic agents to target this important enzyme for disease therapy.

Entities: Chemical Disease Gene Species

Keywords: zzm321990HATzzm321990; HAT1; bisubstrate inhibitor; chemical probes; epigenetics; histone acetyltransferase

Mesh：

Substances：

Year: 2019 PMID： 30637990 PMCID： PMC6533141 DOI： 10.1111/cbdd.13476

Source DB: PubMed Journal: Chem Biol Drug Des ISSN： 1747-0277 Impact factor: 2.817

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