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正在研发用于治疗骨髓纤维化的Janus激酶抑制剂。

Investigational Janus kinase inhibitors in development for myelofibrosis.

作者信息

Bose Prithviraj, Abou Zahr Abdallah, Verstovsek Srdan

机构信息

a Department of Leukemia , University of TX MD Anderson Cancer Center , Houston , TX , USA.

出版信息

Expert Opin Investig Drugs. 2017 Jun;26(6):723-734. doi: 10.1080/13543784.2017.1323871. Epub 2017 May 8.

DOI:10.1080/13543784.2017.1323871
PMID:28441920
Abstract

Since the discovery of the activating V617F mutation in Janus kinase 2 (JAK2), a number of pharmacologic inhibitors of JAK2 have entered clinical trials for patients with myelofibrosis. However, ruxolitinib, approved in 2011, remains the only one currently available for treatment of myelofibrosis, with many others having been discontinued for toxicity, and considerable uncertainty surrounding the future of those still in development. Areas covered: The available clinical data on pacritinib and momelotinib, the two agents in the most advanced phases of clinical testing in myelofibrosis, are examined in detail. NS-018 and INCB039110, selective inhibitors of JAK2 and JAK1, respectively, are also discussed. Finally, the JAK2 inhibitors no longer in clinical development are summarized in tabular form. Expert opinion: The different agents evaluated clearly differ in their kinomes, toxicity profiles and potential for myelosuppression. If approved, the JAK2-specific non-myelosuppressive inhibitor pacritinib could fulfill a major unmet need, that of patients with significant cytopenias. However, toxicity concerns persist. The data from the pivotal trials of momelotinib do not support its approval, although improvement of anemia is an important benefit. Selective JAK1 inhibition alone is unlikely to succeed in myelofibrosis. In these circumstances, rational ruxolitinib-based combinations may represent the best way forward.

摘要

自发现Janus激酶2(JAK2)中的激活型V617F突变以来,多种JAK2的药理抑制剂已进入骨髓纤维化患者的临床试验。然而,2011年获批的鲁索替尼仍是目前唯一可用于治疗骨髓纤维化的药物,许多其他药物因毒性问题已停止研发,而仍在研发中的药物未来发展也存在很大不确定性。涵盖领域:详细研究了帕西替尼和莫美替尼这两种处于骨髓纤维化临床测试最先进阶段的药物的现有临床数据。还讨论了分别为JAK2和JAK1选择性抑制剂的NS-018和INCB039110。最后,以表格形式总结了不再处于临床研发阶段的JAK2抑制剂。专家观点:所评估的不同药物在其激酶组、毒性特征和骨髓抑制潜力方面明显不同。如果获批,JAK2特异性非骨髓抑制性抑制剂帕西替尼可能满足一项重大未满足需求,即患有严重血细胞减少症患者的需求。然而,毒性问题仍然存在。莫美替尼关键试验的数据不支持其获批,尽管改善贫血是一项重要益处。仅选择性抑制JAK1在骨髓纤维化中不太可能成功。在这种情况下,基于鲁索替尼的合理联合用药可能是最佳前进方向。

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