Design of KDM4 Inhibitors with Antiproliferative Effects in Cancer Models.

Young K. Chen,Tiziana Bonaldi,Alessandro Cuomo,Joselyn R. Del Rosario,David J. Hosfield,Toufike Kanouni,Shih-chu Kao,Chon Lai,Neethan A. Lobo,Jennifer Matuszkiewicz,Andrew McGeehan,Shawn M. O’Connell,Lihong Shi,Jeffrey A. Stafford,Ryan Stansfield,James Marvin Veal,Michael S. Weiss,Natalie Y. Yuen,Michael Brennan Wallace

Design of KDM4 Inhibitors with Antiproliferative Effects in Cancer Models.

2017

Young K. Chen
Tiziana Bonaldi
Alessandro Cuomo
Joselyn R. Del Rosario
David J. Hosfield
Toufike Kanouni
Shih-chu Kao
Chon Lai
Neethan A. Lobo
Jennifer Matuszkiewicz
Andrew McGeehan
Shawn M. O’Connell
Lihong Shi
Jeffrey A. Stafford
Ryan Stansfield
James Marvin Veal
Michael S. Weiss
Natalie Y. Yuen
Michael Brennan Wallace

Histone lysine demethylases (KDMs) play a vital role in the regulation of chromatin-related processes. Herein, we describe our discovery of a series of potent KDM4 inhibitors that are both cell permeable and antiproliferative in cancer models. The modulation of histone H3K9me3 and H3K36me3 upon compound treatment was verified by homogeneous time-resolved fluorescence assay and by mass spectroscopy detection. Optimization of the series using structure-based drug design led to compound 6 (QC6352), a potent KDM4 family inhibitor that is efficacious in breast and colon cancer PDX models.

Keywords:

Biology
Drug
Pharmacology
Biochemistry
Colorectal cancer
Cancer
Cell
Homogeneous
Histone
Epigenetics
Oxidoreductase inhibitor

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