SETDB1 Triple Tudor Domain Ligand, (,)-59, Promotes Methylation of Akt1 in Cells

Overview

Journal ACS Chem Biol

Publisher American Chemical Society

Specialties Biochemistry
Biology

Date 2023 Aug 9

PMID 37556795

Authors

Melanie Uguen

Yu Deng

Fengling Li

Devan J Shell

Jacqueline L Norris-Drouin

Michael A Stashko

Suzanne Ackloo

Cheryl H Arrowsmith

Lindsey I James

Pengda Liu

Kenneth H Pearce

Stephen V Frye

Affiliations

Soon will be listed here.

Abstract

Increased expression and hyperactivation of the methyltransferase SET domain bifurcated 1 (SETDB1) are commonly observed in cancer and central nervous system disorders. However, there are currently no reported SETDB1-specific methyltransferase inhibitors in the literature, suggesting that this is a challenging target. Here, we disclose that the previously reported small-molecule ligand for SETDB1's triple tudor domain, (,)-59, is unexpectedly able to increase SETDB1 methyltransferase activity both and in cells. Specifically, (,)-59 promotes SETDB1-mediated methylation of lysine 64 of the protein kinase Akt1. Treatment with (,)-59 also increased Akt1 threonine 308 phosphorylation and activation, a known consequence of Akt1 methylation, resulting in stimulated cell proliferation in a dose-dependent manner. (,)-59 is the first SETDB1 small-molecule positive activator for the methyltransferase activity of this protein. Mechanism of action studies show that full-length SETDB1 is required for significant methylation of an Akt1-K64 peptide and that this activity is stimulated by (,)-59 primarily through an increase in catalytic activity rather than a change in -adenosyl methionine binding.

Citing Articles

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