@article{Arnold Bolomsky_Roy Heusschen_Karin Schlangen_Kathrin Stangelberger_Joséphine Muller_Wolfgang Schreiner_Niklas Zojer_Jo Caers_Heinz Ludwig_2018, place={Pavia, Italy}, title={Maternal embryonic leucine zipper kinase is a novel target for proliferation-associated high-risk myeloma}, volume={103}, url={https://haematologica.org/article/view/8355}, DOI={10.3324/haematol.2017.172973}, abstractNote={Treatment of high-risk patients is a major challenge in multiple myeloma. This is especially true for patients assigned to the gene expression profiling-defined proliferation subgroup. Although recent efforts have identified some key players of proliferative myeloma, genetic interactions and players that can be targeted with clinically effective drugs have to be identified in order to overcome the poor prognosis of these patients. We therefore examined maternal embryonic leucine zipper kinase (MELK) for its implications in hyper-proliferative myeloma and analyzed the activity of the MELK inhibitor OTSSP167 both <em>in vitro</em> and <em>in vivo</em>. <em>MELK</em> was found to be significantly overexpressed in the proliferative subgroup of myeloma. This finding translated into poor overall survival in patients with high <em>vs</em>. low <em>MELK</em> expression. Enrichment analysis of upregulated genes in myeloma cells of <em>MELK</em><sup>high</sup> patients confirmed the strong implications in myeloma cell proliferation. Targeting MELK with OTSSP167 impaired the growth and survival of myeloma cells, thereby affecting central survival factors such as <em>MCL-1</em> and <em>IRF4</em>. This activity was also observed in the 5TGM.1 murine model of myeloma. OTSSP167 reduced bone marrow infiltration and serum paraprotein levels in a dose-dependent manner. In addition, we revealed a strong link between MELK and other proliferation-associated high-risk genes (<em>PLK-1, EZH2, FOXM1, DEPDC1</em&gt;) and MELK inhibition also impaired the expression of those genes. We therefore conclude that MELK is an essential component of a proliferative gene signature and that pharmacological inhibition of MELK represents an attractive novel approach to overcome the poor prognosis of high-risk patients with a proliferative expression pattern.}, number={2}, journal={Haematologica}, author={Arnold Bolomsky and Roy Heusschen and Karin Schlangen and Kathrin Stangelberger and Joséphine Muller and Wolfgang Schreiner and Niklas Zojer and Jo Caers and Heinz Ludwig}, year={2018}, month={Jan.}, pages={325-335} }