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急性髓系白血病的维持治疗:进展与争议。

Maintenance therapy in acute myeloid leukemia: advances and controversies.

机构信息

Department of Leukemia, The University of Texas, MD Anderson Cancer Center.

出版信息

Haematologica. 2023 Sep 1;108(9):2289-2304. doi: 10.3324/haematol.2022.281810.

Abstract

The last decade has seen steadfast progress in drug development in acute myeloid leukemia (AML) which has moved progressively towards genomic-based therapy. With these advances, outcomes in AML have improved but remains far from satisfactory. One approach towards preventing relapse in AML is to use maintenance therapy in patients, after attaining remission. Allogeneic hematopoietic stem cell transplantation (HSCT) is an effective post-remission therapy that has been proven to reduce the risk of relapse. However, in patients who are ineligible for HSCT or have a high risk of relapse, other effective measures to prevent relapse are needed. There is also a need for post-HSCT maintenance to reduce relapse in high-risk subsets. Over the last 3 decades maintenance therapy in AML has evolved from the use of chemotherapeutic agents to more targeted therapies and better modulation of the immune system. Unfortunately, improvements in survival outcomes as a result of using these agents have not been consistently demonstrated in clinical trials. To derive the optimum benefit from maintenance therapy the time points of therapy initiation need to be defined and therapy must be selected precisely with respect to the AML genetics and risk stratification, prior treatment exposure, transplant eligibility, expected toxicity and the patient's clinical profile and desires. The far-reaching goal is to facilitate patients with AML in remission to achieve a normal quality of life while improving remission duration and overall survival. The QUAZAR trial was a welcome step towards a safe maintenance drug that is easy to administer and showed survival benefit but leaves many open issues for discussion. In this review we will discuss these issues, highlighting the development of AML maintenance therapies over the last 3 decades.

摘要

过去十年,急性髓系白血病(AML)的药物研发取得了稳步进展,逐步向基于基因组的治疗方法发展。随着这些进展,AML 的治疗结果有所改善,但仍远未令人满意。预防 AML 复发的一种方法是在患者达到缓解后使用维持治疗。异基因造血干细胞移植(HSCT)是一种有效的缓解后治疗方法,已被证明可降低复发风险。然而,对于不适合 HSCT 或复发风险高的患者,需要其他有效的预防复发措施。此外,还需要进行 HSCT 后的维持治疗,以降低高危亚组的复发风险。在过去的 30 年中,AML 的维持治疗已从使用化疗药物发展为更具针对性的治疗方法和更好地调节免疫系统。不幸的是,临床试验并未一致证明这些药物的使用可改善生存结果。为了从维持治疗中获得最佳获益,需要确定治疗开始的时间点,并且必须根据 AML 的遗传学和风险分层、先前的治疗暴露、移植资格、预期毒性以及患者的临床特征和意愿,精确选择治疗药物。最终目标是帮助缓解期的 AML 患者实现正常的生活质量,同时延长缓解期和总生存期。QUAZAR 试验是朝着安全的维持药物迈出的可喜一步,这种药物易于管理且具有生存获益,但仍有许多问题需要讨论。在这篇综述中,我们将讨论这些问题,重点介绍过去 30 年来 AML 维持治疗的发展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8e2e/10483353/6de52a46c3dd/1082289.fig1.jpg

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