Fragment-Based Discovery of Type I Inhibitors of Maternal
Embryonic Leucine Zipper Kinase

Andrew Sharff (219769); Christopher C. F. Hamlett (1693489); Christopher N. Johnson (157130); David
C. Rees (1693507); Dirk Brehmer (844425); Eddy J. E. Freyne (1693498); François Sommen (1464823); Joannes T. M. Linders (844424); Joseph E. Coyle (1668076); Lieven Meerpoel (1457320); Lijs Beke (1693501); Martyn Frederickson (1693480); Pascal Bonnet (439270); Phillip J. Day (1668073); Rachel McMenamin (1693477); Ron A. H. J. Gilissen (1693486); Sahil Patel (1668058); Steven Howard (760049); Tongfei Wu (1693510); Valerio Berdini (1668088)

Fragment-Based Discovery of Type I Inhibitors of Maternal Embryonic Leucine Zipper Kinase

Abstract

Fragment-based drug design was successfully applied to maternal embryonic leucine zipper kinase (MELK). A low affinity (160 μM) fragment hit was identified, which bound to the hinge region with an atypical binding mode, and this was optimized using structure-based design into a low-nanomolar and cell-penetrant inhibitor, with a good selectivity profile, suitable for use as a chemical probe for elucidation of MELK biology

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Last time updated on 12/02/2018