Discovery of Potent, Selective, and Structurally Novel Dot1L Inhibitors by a Fragment Linking Approach

Henrik Möbitz,Rainer Machauer,Philipp Holzer,Andrea Vaupel,Frédéric Stauffer,Christian Ragot,Giorgio Caravatti,Clemens Scheufler,César Fernández,Ulrich Hommel,Ralph Tiedt,Kim S. Beyer,Chao Chen,Hugh Zhu,Christoph Gaul

Discovery of Potent, Selective, and Structurally Novel Dot1L Inhibitors by a Fragment Linking Approach

2017

Henrik Möbitz
Rainer Machauer
Philipp Holzer
Andrea Vaupel
Frédéric Stauffer
Christian Ragot
Giorgio Caravatti
Clemens Scheufler
César Fernández
Ulrich Hommel
Ralph Tiedt
Kim S. Beyer
Chao Chen
Hugh Zhu
Christoph Gaul

Misdirected catalytic activity of histone methyltransferase Dot1L is believed to be causative for a subset of highly aggressive acute leukemias. Targeting the catalytic domain of Dot1L represents a potential therapeutic approach for these leukemias. In the context of a comprehensive Dot1L hit finding strategy, a knowledge-based virtual screen of the Dot1L SAM binding pocket led to the discovery of 2, a non-nucleoside fragment mimicking key interactions of SAM bound to Dot1L. Fragment linking of 2 and 3, an induced back pocket binder identified in earlier studies, followed by careful ligand optimization led to the identification of 7, a highly potent, selective and structurally novel Dot1L inhibitor.

Keywords:

Biology
Biochemistry
DOT1L
MIXED LINEAGE LEUKEMIA
Ligand
Protein Lysine Methyltransferase
Histone methyltransferase DOT1L
Transferase
virtual screen
binding pocket

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