对于慢性或加速期CML,其他治疗方案可能会将奥美西辛降级为最后一线选择

M. Kalaycio
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引用次数: 0

摘要

许多肿瘤学家都记得同源山楂酸酯碱(HHT)的传奇历史,并想知道它到底发生了什么。HHT对髓性白血病,特别是慢性髓性白血病(CML)显示出初步的希望,在慢性髓性白血病(CML)中,HHT似乎比干扰素α诱导更多的细胞遗传学缓解。对HHT研究者来说不幸的是,但对其他人来说幸运的是,这些研究与伊马替尼的研究是一致的。伊马替尼的显著引入促成了20世纪90年代中后期HHT的搁置。然而,伊马替尼通常并不完美。一些CML患者产生耐药性,其中大约一半是通过获得结合位点突变而产生的。特别是一种突变,T315I,使CML患者对所有可用的酪氨酸激酶抑制剂(TKI)具有耐药性。与此同时,一种半合成的HHT,甲琥珀酸奥乙辛,被开发出来。在业界合作伙伴的帮助下,MD安德森癌症中心的研究人员开始了对奥米克辛治疗TKI耐药CML患者的新研究。在62例T315I突变的CML患者中,77%的患者获得完全血液学缓解,中位缓解持续时间为9.1个月。此外,在部分患者中也实现了细胞遗传学应答,完成率为16%。这些数据促使fda批准了这一申请,但由于缺乏T315I突变的标准化测试而被拒绝。Community Translations第194页文章中提供的额外数据构成了第二次申请的基础,这一次是针对对2个或更多tki耐药的CML患者的适应症。这些数据证明了奥米克辛对晚期CML患者的安全性。骨髓抑制是迄今为止最常见和最严重的毒性治疗。骨髓抑制可能是延迟的和深刻的。否则,皮下注射耐受性良好。Omacetaxine的疗效一般,慢性期CML患者有18%-20%的主要细胞遗传学反应,而加速期CML患者没有。血液学反应更为频繁,临床实践中,奥乙酰辛的一个明显作用是,当患者正在接受二线或三线TKI治疗时,作为异基因移植的治疗桥梁。还有其他角色吗?口服第三代TKI ponatinib在对两种或两种以上其他TKI耐药后也具有活性,即使存在T315I突变,这表明当所有或大多数TKI已经尝试过时,omacetaxine将被归为最后一线治疗。即便如此,在没有移植计划的情况下,治疗目标很大程度上是姑息性的,因为奥美乙辛诱导的细胞遗传学反应持续时间相对较短(中位数为12个月)。羟基脲可能提供更方便和更便宜的姑息。目前,奥乙辛的所有其他作用都处于研究阶段。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Other therapy options may relegate omacetaxine to last-line choice for chronic or accelerated phase CML
Many oncologists remember the storied history of homoharringtonine (HHT) and wonder whatever happened to it. HHT showed initial promise for myeloid leukemias, particularly for chronic myelogenous leukemia (CML) where it seemed to induce more cytogenetic remissions than did interferon alpha. Unfortunately for HHT investigators, but fortunately for everybody else, these studies coincided with those being done with imatinib. The phenomenal introduction of imatinib contributed to the shelving of HHT in the mid to late 1990s. As is often the case, though, imatinib is not perfect. Some patients with CML develop resistance and approximately half of these do so through the acquisition of binding site mutations. One mutation in particular, T315I, rendered patients with CML resistant to all available tyrosine kinase inhibitors (TKI). In the meantime, a semisynthetic version of HHT, omacetaxine mepesuccinate, was developed. With the help of partners in industry, investigators at MD Anderson Cancer Center initiated new studies of omacetaxine in TKI resistant CML patients. Among 62 CML patients with a T315I mutation, complete hematologic response was achieved in 77% with median response duration of 9.1 months. Further, cytogenetic response was also achieved in a portion of patients, complete in 16%. These data prompted application for approval by the Food and Drug Administration, but were rejected for lack of a standardized test for T315I mutations. The additional data presented in the Community Translations article on page 194 formed the basis of a second application, this time for an indication in patients with CML resistant to 2 or more TKIs. The data speak to omacetaxine’s safety in patients with advanced CML. Myelosuppression is by far the most common and serious toxicity of treatment. The myelosuppression may be delayed and profound. Otherwise, the subcutaneous injections are well tolerated. Omacetaxine’s efficacy is modest with 18%-20% major cytogenetic response in CML patients in chronic phase but none in those in accelerated phase. Hematologic responses were more frequent and one obvious role for omacetaxine in clinical practice is as a therapeutic bridge to allogeneic transplant when patients are progressing on secondor third-line TKI therapy. Are there any other roles? The availability of an orally administered third-generation TKI, ponatinib, that is also active after resistance to two or more other TKIs, even when the T315I mutation is present, suggests that omacetaxine will be relegated to last-line therapy when all or most TKIs have already been tried. Even then, in the absence of a plan for transplant, treatment goals are largely palliative since the cytogenetic responses induced by omacetaxine are of relatively short duration (median, 12 months). Hydroxyurea may provide more convenient and less expensive palliation. All other roles for omacetaxine are currently investigational.
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