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Článek

Pevonedistat, a NEDD8-activating enzyme inhibitor, is active in mantle cell lymphoma and enhances rituximab activity in vivo

Czuczman, Natalie M
Autor Czuczman, Natalie M Department of Pediatrics, Departments of Medicine and Immunology
Barth, Matthew J
Autor Barth, Matthew J Department of Pediatrics, Departments of Medicine and Immunology
Gu, Juan
Autor Gu, Juan Departments of Medicine and Immunology
Neppalli, Vishala
Autor Neppalli, Vishala Department of Pathology, and
Mavis, Cory
Autor Mavis, Cory Departments of Medicine and Immunology
Frys, Sarah E
Autor Frys, Sarah E Department of Pediatrics, Departments of Medicine and Immunology
Hu, Qiang
Autor Hu, Qiang Department of Biostatistics and Bioinformatics, Roswell Park Cancer Institute, Buffalo, NY;
Liu, Song
Autor Liu, Song Department of Biostatistics and Bioinformatics, Roswell Park Cancer Institute, Buffalo, NY;
Klener, Pavel
Autor Klener, Pavel Department of Pediatrics, University of Buffalo, Buffalo, NY; and Clinical Department of Hematology, Institute of Pathophysiology, Charles University in Prague, Prague, Czech Republic
Vockova, Petra
Autor Vockova, Petra Department of Pediatrics, University of Buffalo, Buffalo, NY; and Clinical Department of Hematology, Institute of Pathophysiology, Charles University in Prague, Prague, Czech Republic

Blood. 2016 Mar 03 ; 127 (9) : 1128-37. [epub] 20151216

ISSN 1528-0020 | 0006-4971
Zdroj

Mantle cell lymphoma (MCL) is characterized by an aggressive clinical course and inevitable development of refractory disease, stressing the need to develop alternative therapeutic strategies. To this end, we evaluated pevonedistat (MLN4924), a novel potent and selective NEDD8-activating enzyme inhibitor in a panel of MCL cell lines, primary MCL tumor cells, and 2 distinct murine models of human MCL. Pevonedistat exposure resulted in a dose-, time-, and caspase-dependent cell death in the majority of the MCL cell lines and primary tumor cells tested. Of interest, in the MCL cell lines with lower half-maximal inhibitory concentration (0.1-0.5 μM), pevonedistat induced G1-phase cell cycle arrest, downregulation of Bcl-xL levels, decreased nuclear factor (NF)-κB activity, and apoptosis. In addition, pevonedistat exhibited additive/synergistic effects when combined with cytarabine, bendamustine, or rituximab. In vivo, as a single agent, pevonedistat prolonged the survival of 2 MCL-bearing mouse models when compared with controls. Pevonedistat in combination with rituximab led to improved survival compared with rituximab or pevonedistat monotherapy. Our data suggest that pevonedistat has significant activity in MCL preclinical models, possibly related to effects on NF-κB activity, Bcl-xL downregulation, and G1 cell cycle arrest. Our findings support further investigation of pevonedistat with or without rituximab in the treatment of MCL.

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