急性早幼粒细胞白血病治愈性治疗后的治疗相关髓样肿瘤:发病率、与治疗方案的相关性和未来方向

Pub Date : 2024-09-10 DOI:10.1007/s12308-024-00606-6
Adil Menon, Madina Sukhanova, Juehua Gao, Kristy Wolniak, Lucy Fu, Yi-Hua Chen, Qing Ching Chen, Hamza Tariq
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引用次数: 0

摘要

全反式维甲酸(ATRA)和三氧化二砷(ATO)彻底改变了急性早幼粒细胞白血病(APL)的治疗,治愈率高达 80%。在提高生存率的同时,抗 APL 疗法的长期后果也日益明显,其中包括潜在的治疗相关髓样肿瘤(t-MNs)。众所周知,细胞毒性化疗后会产生髓细胞肿瘤,但只使用 ATRA/ATO 的治疗方案的致白血病潜力尚未得到充分证实。本研究旨在探讨抗 APL 治疗后出现的 t-MNs 的发病率、长期风险和临床病理特征,以及它们与所采用的治疗方案之间的相关性。我们回顾性地收集了 2001 年 1 月至 2021 年 2 月期间接受治疗的 APL 患者,根据所采用的治疗方案将其分为 ATRA/ATO + 化疗组和 ATRA/ATO 组,并评估了 t-MN 的发生情况。共确定了 110 例 APL 患者,其中 67 例(61%)接受了 ATRA/ATO + 化疗,43 例(39%)仅接受了 ATRA/ATO 治疗。总体而言,4/110(3.6%)名患者出现了t-MNs,所有四名患者均出现在ATRA/ATO+化疗组。最终,ATRA/ATO + 化疗组的 t-MN 发生率明显高于仅接受 ATRA/ATO 治疗组(分别为 5.97% 对 0.0%;P = 0.0289)。我们二十多年来的数据表明,APL 的常规化疗与发生 t-MN 的微小但重要的风险有关,而 ATR/ATO 则没有这种风险。考虑到最近和正在进行的几项试验表明,在不久的将来,无化疗方法对所有风险 APL 类型都是可行的,这就具有了新的意义。因此,在 APL 治疗方案中省略致白血病的化疗(也可以说是不必要的化疗),可能会降低长期存活者的 t-MN 发生率,而不会影响其治愈率。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Therapy-related myeloid neoplasms following curative treatment of acute promyelocytic leukemia: incidence, correlation with therapeutic regimen, and future directions

All-trans retinoic acid (ATRA) and arsenic trioxide (ATO) have revolutionized the treatment of acute promyelocytic leukemia (APL), offering a cure rate of > 80%. Along with improved survival, the long-term consequences of anti-APL therapy are becoming increasingly apparent, including potential therapy-related myeloid neoplasms (t-MNs). T-MNs are well known to arise after cytotoxic chemotherapy, but the leukemogenic potential of regimens utilizing only ATRA/ATO is not well established. The objective of this study is to examine the incidence, long-term risk, and clinicopathologic features of t-MNs arising after anti-APL therapy and how they correlates with the therapeutic regimen employed. We retrospectively collected treated APL patients between 01/2001 and 02/2021, categorized them into ATRA/ATO + chemo and ATRA/ATO groups based on the regimen used, and evaluated for the development of t-MN. A total of 110 APL patients were identified, including 67 (61%) treated with ATRA/ATO + chemo and 43 (39%) treated with ATRA/ATO only. Overall, 4/110 (3.6%) patients developed t-MNs, with all four emerging in the ATRA/ATO + chemo group. Ultimately, the incidence of t-MN in ATRA/ATO + chemo group was significantly higher compared with ATRA/ATO only group(5.97% vs. 0.0%, respectively; p = 0.0289). Our data spanning over two decades suggests that conventional chemotherapy for APL is associated with a small but significant risk of t-MN, whereas ATR/ATO does not carry this risk. This takes on new significance, considering several recent and ongoing trials have shown that a chemotherapy-free approach might become feasible for all risk APL types in the near future. Consequently, the omission of leukemogenic and arguably unnecessary chemotherapy from APL regimens may reduce the incidence of t-MNs in long-term survivors without sacrificing their cure rates.

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