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Is molecular remission the goal of multiple myeloma therapy?

机译:分子缓解多发性骨髓瘤治疗的目标是什么?

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The increased number of effective therapies and the wider use of combinations that give deeper remissions have resulted in a reassessment of the goals of myeloma therapy. With the advent of new therapeutic strategies and diagnostic tools, achievement of minimal residual disease (MRD)-negative status has become increasingly important, with some even considering it as the primary endpoint for therapy. The level of MRD that is aimed for is a continuous, rather than an absolute variable, with studies in both transplant-eligible and -noneligible patients showing that the level of MRD achieved is predictive of progression-free survival and overall survival, with an improvement in survival of approximately 1 year for each log-depletion in MRD level. The most widely used methods to assess MRD status include flow cytometry and clonality detection, using next-generation sequencing technologies with sensitivity limits of 1:10~(?3) to 1:10~(?6). The timing of when to assess MRD depends on the treatment used, as well as the molecular and cytogenetic subgroup of the myeloma itself. It is also becoming clear that the level of MRD negativity, as well as microenvironmental factors, are important prognostically, including the regeneration of normal plasma cells, and the normalization of the immune repertoire. With advances in antibody-based therapy and immunotherapy, the achievement of stable MRD states is now possible for a significant proportion of patients, and is a prerequisite for myeloma cure.
机译:有效疗法的数量增加和更广泛地使用给予更深的缓解的组合使得重新评估骨髓瘤治疗的目标。随着新的治疗策略和诊断工具的出现,实现最小的残留疾病(MRD) - 负面地位越来越重要,一些甚至认为它是治疗的主要终点。旨在的MRD水平是连续而不是绝对变量,具有移植符合条件的和不合格的患者的研究表明,达到的MRD水平是可预测无进展的生存和整体生存率,具有改善在MRD级别的每个对数耗尽的存活率为约1年。使用最广泛的评估MRD状态的方法包括流式细胞术和克隆性检测,利用具有1:10〜(?3)至1:10〜(?6)的灵敏度限制的下一代测序技术。何时评估MRD的时间取决于所用的处理,以及骨髓瘤本身的分子和细胞遗传学亚组。显然,MRD消极性以及微环境因素的程度也很重要,预后,包括正常血浆细胞的再生,以及免疫曲目的标准化。随着基于抗体的治疗和免疫疗法的进展,现在可以实现稳定的MRD状态的成就,这是一部分患者,并且是骨髓瘤治疗的先决条件。

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    《Hematology》 |2017年第1期|共7页
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