Issue 7, 2019

Selectivity, ligand deconstruction, and cellular activity analysis of a BPTF bromodomain inhibitor

Abstract

Bromodomain and PHD finger containing protein transcription factor (BPTF) is an epigenetic protein involved in chromatin remodelling and is a potential anticancer target. The BPTF bromodomain has one reported small molecule inhibitor (AU1, rac-1). Here, advances made on the structure–activity relationship of a BPTF bromodomain ligand are reported using a combination of experimental and molecular dynamics simulations leading to the active enatiomer (S)-1. Additionally, a ligand deconstruction analysis was conducted to characterize important pharmacophores for engaging the BPTF bromodomain. These studies have been enabled by a protein-based fluorine NMR approach, highlighting the versatility of the method for selectivity, ligand deconstruction, and ligand binding. To enable future analysis of biological activity, cell growth analyses in a panel of cancer cell lines were carried out using CRISPR-Cas9 and (S)-1 to identify cell-based model systems that are sensitive to BPTF inhibition.

Graphical abstract: Selectivity, ligand deconstruction, and cellular activity analysis of a BPTF bromodomain inhibitor

Supplementary files

Article information

Article type
Paper
Submitted
20 окт. 2018
Accepted
23 јан. 2019
First published
25 јан. 2019

Org. Biomol. Chem., 2019,17, 2020-2027

Selectivity, ligand deconstruction, and cellular activity analysis of a BPTF bromodomain inhibitor

S. E. Kirberger, P. D. Ycas, J. A. Johnson, C. Chen, M. F. Ciccone, R. W. L. Woo, A. K. Urick, H. Zahid, K. Shi, H. Aihara, S. D. McAllister, M. Kashani-Sabet, J. Shi, A. Dickson, C. O. dos Santos and W. C. K. Pomerantz, Org. Biomol. Chem., 2019, 17, 2020 DOI: 10.1039/C8OB02599A

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