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Suboptimal Response to or Failure of Imatinib Treatment for Chronic Myeloid Leukemia: What Is the Optimal Strategy?

机译:对伊马替尼治疗慢性粒细胞白血病的反应欠佳或失败:最佳策略是什么?

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摘要

Treatment responses to imatinib vary among patients with chronic myeloid leukemia (CML), and definitions of treatment failure and suboptimal response have been published. This article discusses monitoring and treatment of patients with CML after failure of or suboptimal response to imatinib therapy. We reviewed articles listed on PubMed from January 1, 2002, to July 31, 2008, and abstracts from the 2007 Annual Meeting of the American Society of Hematology. Search terms used were chronic myeloid/myelogenous leukemia, imatinib, and BCR-ABL. To enable early recognition of suboptimal responses, patients should be frequently monitored according to published guidelines, including cytogenetic analysis every 6 months until a complete response is achieved and molecular monitoring every 3 months from the start of therapy or monthly if an increasing BCR-ABL1 transcript level is detected. Mutational analysis of BCR-ABL1 may assist with treatment selection. A recent survey suggests that a notable proportion of physicians do not follow treatment guidelines and that broader communication is required. Recent recommendations state that, in patients whose response to imatinib at 400 mg/d is suboptimal, the dose should be increased, whereas alternative therapies, such as dasatinib, nilotinib, and allogeneic stem cell transplant (in eligible patients), and imatinib dose escalation should be considered after imatinib failure. However, clinical data are lacking to confirm this sequence of treatments, and introducing alternative therapies at an earlier stage of treatment, for example, after a suboptimal response, may produce better long-term outcomes in a higher proportion of patients. Patient and disease characteristics should be carefully considered to optimize treatment strategy for CML.
机译:慢性粒细胞白血病(CML)患者对伊马替尼的治疗反应各不相同,并且治疗失败和次优反应的定义也已发表。本文讨论对伊马替尼治疗失败或反应欠佳后的CML患者的监测和治疗。我们回顾了2002年1月1日至2008年7月31日在PubMed上列出的文章,以及美国血液学会2007年年会的摘要。使用的搜索词是慢性髓样/骨髓性白血病,伊马替尼和BCR-ABL。为了能够及早识别出次优反应,应根据已发布的指南对患者进行频繁监测,包括每6个月进行一次细胞遗传学分析直至获得完全的反应,从治疗开始或每3个月进行分子监测(如果BCR-ABL1转录本增加)水平被检测到。 BCR-ABL1的突变分析可能有助于治疗选择。最近的一项调查表明,显着比例的医生未遵循治疗指南,因此需要更广泛的沟通。最近的建议指出,对于400 mg / d的伊马替尼反应不理想的患者,应增加剂量,而替代疗法,如达沙替尼,尼罗替尼和同种异体干细胞移植(在合格患者中),以及伊马替尼剂量递增伊马替尼治疗失败后应考虑。但是,缺乏临床数据来确认这种治疗顺序,并且在较早的治疗阶段(例如,反应欠佳之后)引入替代疗法可能会在更高比例的患者中产生更好的长期疗效。应仔细考虑患者和疾病特征,以优化CML的治疗策略。

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