Alisertib (MLN8237), an Oral Selective Inhibitor of Aurora Kinase a, Has Clinical Activity and Restores GATA1 Expression in Patients with Myelofibrosis

Gangat, Naseema; Stein, Brady L.; Marinaccio, Christian; Swords, Ronan; Watts, Justin M.; Gurbuxani, Sandeep; Frankfurt, Olga; Altman, Jessica K.; Wen, Jeremy Q.; Farnoud, Noushin; Famulare, Christopher; Patel, Akshar; Tapia, Roberto; Handlogten, Amy; Dinh, Yvonne; Englund, Kristen; Patel, Shradha; Nobrega, Juan Carlos; Tejera, Dalissa; Thomassen, Amber; Stein, Harald; Gao, Juehua; Ji, Peng; Rampal, Raajit K.; Giles, Francis J.; Tefferi, Ayalew; Crispino, John D.

doi:10.1182/blood-2018-99-110381

Cited by 9 publications

(3 citation statements)

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“…In a phase 1 study of higher-risk MF patients, treatment with the AURKA inhibitor alisertib led to a spleen response in 29% (4 of 14), transfusion independence in 8% (1 of 13), and $50% symptom improvement in 23% (5 of 22) of patients. 36 In addition to restoring GATA1 expression in megakaryocytes, a 1-grade reduction if fibrosis score was observed in 4 of 6 patients with paired samples.…”

Section: Other Pathways and Targets In Mpnsmentioning

confidence: 96%

Beyond JAK-STAT: novel therapeutic targets in Ph-negative MPN

Gerds

2019

Hematology

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The Philadelphia chromosome-negative myeloproliferative neoplasms (MPNs) share a common pathobiology of constitutive activation of the JAK and STAT pathway, despite having the 3 distinct phenotypes of essential thrombocythemia, polycythemia vera, and primary myelofibrosis. Targeting the JAK-STAT pathway has led to remarkable clinical benefit, including reduction in splenomegaly, amelioration of cytokine-driven symptoms, improvement in quality of life, and even some improvement in survival. However, targeting this pathway has not resulted in consistent disease modification by current metrics, including a reduction in mutant allele burden or reversal of fibrosis. Moreover, targeting JAK-STAT can lead to limiting treatment-emergent side effects, such as anemia and thrombocytopenia. Continued discovery points to a complex system of pathogenesis beyond JAK-STAT driving the formation and evolution of MPNs. This article reviews the successes and limitations of JAK-STAT inhibition, surveys the strategies behind emerging therapies, and discusses the challenges that are present in moving beyond JAK-STAT.

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Section: Other Pathways and Targets In Mpnsmentioning

confidence: 96%

Beyond JAK-STAT: novel therapeutic targets in Ph-negative MPN

Gerds

2019

Hematology

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“…A selective aurora kinase-alpha inhibitor, alisertib, eradicates atypical megakaryocytes and reduces marrow fibrosis. Alisertib was found to reduce splenomegaly and symptom burden in 29% and 32% of patients with MF, respectively, during a phase II clinical study, it also normalizes megakaryocytes reducing fibrosis in 5 of 7 patients [81,96].…”

Section: Inhibitors Of Fibrosismentioning

confidence: 97%

Mutational Analysis of Driver and Non-driver Mutations of Philadelphia Chromosome-negative Myeloproliferative Neoplasms; Diagnosis and Recent Advances in Treatment

Afolabi,

Riwaz,

Weerasena

et al. 2024

WJCOR

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Myeloproliferative neoplasms (MPNs) are hematological disorders affecting myeloid stem cells. They are classified as Philadelphia (Ph) chromosome positive-chronic myeloid leukemia, and Ph-negative polycythemia vera, essential thrombocythemia, primary myelofibrosis, chronic neutrophilic leukemia, chronic eosinophilic leukemia, juvenile myelomonocytic leukemia, and MPN unclassifiable. This review is mainly focused on the Ph-negative MPNs namely, PV, ET, and PMF. These affect both males and females with a slight male predominance, with patients mainly presenting in the seventh decade. Patients often present with thrombotic events resulting in complications that lower survival rates. The major driver mutations that have been identified in MPNs are JAK2 Exon 14, JAK2 Exon 12, MPL Exon 10, and CALR Exon 9. The importance of these driver mutations gives due recognition to their inclusion into the 2022 diagnostic criteria of the MPN WHO Classification. However, other non-driver mutations have also been reported, especially in triple-negative cases. These mutations lead to downstream constitutive activation of the JAK/STAT signaling pathway, as well as the MAPK, and PI3K/Akt pathways. Insights into the molecular pathogenesis of MPN and its association with JAK2, CALR, and MPL mutations have identified JAK2 as a rational therapeutic target. Thus, as an approach to MPN therapy, JAK2 inhibitors, such as ruxolitinib, have been shown to effectively inhibit JAK2, and are currently in clinical trials in combination with other drug classes. This review comprehensively examines the molecular markers of the main Ph-negative MPNs, as well as diagnosis and treatment options.

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“…The link between driver mutations, alterations of megakaryocyte maturation, and disease progression in MF has been recently clarified by the observations that mice expressing JAK2 V617F only in megakaryocytes develop MF 114 ; the driver mutations induce a ribosomopathy that reduces the content of the transcription factor GATA1 (which is essential for terminal maturation) in megakaryocytes, halting their maturation 115, 116 ; mice lacking the regulatory sequences which specifically drive GATA1 expression in megakaryocytes ( Gata1 low mice) develop the same megakaryocyte abnormalities observed in MF and MF with age 117, 118 ; and, finally, treatment with an inhibitor of Aurora kinase A, a protein overexpressed in MF megakaryocytes, rescues GATA1 expression in these cells, curing MF in animal models 119 , suggesting GATA1 as a druggable target in MF 120 . This clinical hypothesis was tested by demonstrating that an inhibitor of Aurora Kinase A has some efficacy in MF patients 121 . Owing to these exciting results, additional megakaryocyte abnormalities are currently being considered as potential therapeutic targets for MF.…”

Section: Harnessing the Altered P53–tgf-β Circuitry To Treat Mfmentioning

confidence: 99%

Novel strategies for the treatment of myelofibrosis driven by recent advances in understanding the role of the microenvironment in its etiology

et al. 2019

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Myelofibrosis is the advanced stage of the Philadelphia chromosome-negative myeloproliferative neoplasms (MPNs), characterized by systemic inflammation, hematopoietic failure in the bone marrow, and development of extramedullary hematopoiesis, mainly in the spleen. The only potentially curative therapy for this disease is hematopoietic stem cell transplantation, an option that may be offered only to those patients with a compatible donor and with an age and functional status that may face its toxicity. By contrast, with the Philadelphia-positive MPNs that can be dramatically modified by inhibitors of the novel BCR-ABL fusion-protein generated by its genetic lesion, the identification of the molecular lesions that lead to the development of myelofibrosis has not yet translated into a treatment that can modify the natural history of the disease. Therefore, the cure of myelofibrosis remains an unmet clinical need. However, the excitement raised by the discovery of the genetic lesions has inspired additional studies aimed at elucidating the mechanisms driving these neoplasms towards their final stage. These studies have generated the feeling that the cure of myelofibrosis will require targeting both the malignant stem cell clone and its supportive microenvironment. We will summarize here some of the biochemical alterations recently identified in MPNs and the novel therapeutic approaches currently under investigation inspired by these discoveries.

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Alisertib (MLN8237), an Oral Selective Inhibitor of Aurora Kinase a, Has Clinical Activity and Restores GATA1 Expression in Patients with Myelofibrosis

Cited by 9 publications

References 0 publications

Beyond JAK-STAT: novel therapeutic targets in Ph-negative MPN

Beyond JAK-STAT: novel therapeutic targets in Ph-negative MPN

Mutational Analysis of Driver and Non-driver Mutations of Philadelphia Chromosome-negative Myeloproliferative Neoplasms; Diagnosis and Recent Advances in Treatment

Novel strategies for the treatment of myelofibrosis driven by recent advances in understanding the role of the microenvironment in its etiology

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