Clinical potential of midostaurin in advanced systemic mastocytosis

IF 3.9 Q2 ONCOLOGY
M. Chandesris, G. Damaj, O. Lortholary, O. Hermine
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引用次数: 0

Abstract

Advanced (Ad) systemic mastocytoses (SM) include aggressive SM (ASM) and mast cell leukemia (MCL) with or without an associated clonal hematological non-mast cell lineage disease (AHNMD). They are rare (<15%) but are associated with a poor prognosis due to rapid organ dysfunction. To date, responses to high-dose chemotherapy, cladribine, and imatinib were revealed to be suboptimal with a median survival time of 24 months. Midostaurin is a potent multikinase inhibitor including the most frequent KIT D816V mutation (>80%). We herein present a review of the most recent data of the use of midostaurin in AdSM. First, a multicenter Phase II study (CPKC412D2213) revealed an unprecedented overall response rate (ORR) of 69% regardless of KIT mutational status, with 38% of major response (MR) among 26 AdSM patients treated with midostaurin alone 200 mg daily. Second, a sponsor-initiated, multicenter, single-arm open Phase II study (CPKC412D2201) confirmed a high and durable ORR of 60% including 45% of MR among 89 AdSM patients. Finally, a French compassionate use program managed by the French Reference Centre for Mastocytosis allowed the treatment of almost a hundred AdSM patients to date in France since the CPKC412D2201 study closure. The outcome of the first 28 treated patients under cover of this on-going procedure revealed an ORR of 71% including 57% of MR. Most importantly, survival analysis revealed in comparison to a historical control cohort of AdSM patients who did not receive midostaurin a twofold lower risk of death (p=0.02) in midostaurin-treated patients. Side effects revealed were acceptable and manageable (mostly digestive). Midostaurin appears to be an effective and safe treatment of AdSM. However, its effect on the course of the AHNMD is less clear. For the future, combined therapy (hypomethylating agents, cladribine, mammalian target of rapamycin inhibitors, chemotherapy, and allogeneic bone marrow transplantation) may further improve long-term survival, particularly that of MCL and AdSM patients with AHNMD.
midoin治疗晚期全身肥大细胞增多症的临床潜力
晚期(Ad)系统性肥大细胞病(SM)包括侵袭性SM (ASM)和肥大细胞白血病(MCL),伴或不伴克隆性血液学非肥大细胞谱系疾病(AHNMD)。他们很少见(80%)。在此,我们对midosvin在AdSM中使用的最新数据进行了回顾。首先,一项多中心II期研究(CPKC412D2213)显示,无论KIT突变状态如何,总缓解率(ORR)都达到了前所未有的69%,在26名AdSM患者中,每天单独使用200毫克米多斯汀治疗,主要缓解率(MR)为38%。其次,一项由发起人发起的多中心单臂开放式II期研究(CPKC412D2201)证实,89例AdSM患者的ORR高且持久,为60%,其中MR为45%。最后,自CPKC412D2201研究结束以来,由法国肥大细胞增多症参考中心管理的法国同情使用项目允许在法国治疗近100名AdSM患者。最重要的是,生存分析显示,与未接受米多斯汀治疗的AdSM患者的历史对照队列相比,接受米多斯汀治疗的患者的死亡风险降低了两倍(p=0.02)。显示的副作用是可以接受和可控的(主要是消化)。米多舒林似乎是一种有效和安全的治疗AdSM的方法。然而,它对AHNMD病程的影响尚不清楚。未来,联合治疗(低甲基化药物、克拉德滨、哺乳动物靶向雷帕霉素抑制剂、化疗和异体骨髓移植)可能会进一步提高长期生存率,特别是MCL和AdSM合并AHNMD患者。
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来源期刊
自引率
7.10%
发文量
16
审稿时长
16 weeks
期刊介绍: Blood and Lymphatic Cancer: Targets and Therapy is an international, peer reviewed, open access journal focusing on blood and lymphatic cancer research, identification of therapeutic targets, and the optimal use of preventative and integrated treatment interventions to achieve improved outcomes, enhanced survival, and quality of life for the cancer patient. Specific topics covered in the journal include: Epidemiology, detection and screening Cellular research and biomarkers Identification of biotargets and agents with novel mechanisms of action Optimal clinical use of existing anticancer agents, including combination therapies Radiation, surgery, bone marrow transplantation Palliative care Patient adherence, quality of life, satisfaction Health economic evaluations.
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