慢性期慢性髓性白血病的深度分子反应率:Gimema Labnet CML 国家网络经验中与反应时间和不同前线 TKI 相关的停药资格。

IF 2.7 4区 医学 Q2 HEMATOLOGY
Massimo Breccia, Rosalba Cucci, Giovanni Marsili, Fausto Castagnetti, Sara Galimberti, Barbara Izzo, Federica Sorà, Simona Soverini, Monica Messina, Alfonso Piciocchi, Massimiliano Bonifacio, Daniela Cilloni, Alessandra Iurlo, Giovanni Martinelli, Gianantonio Rosti, Fabio Stagno, Paola Fazi, Marco Vignetti, Fabrizio Pane
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引用次数: 0

摘要

背景:在过去十年中,TKIs 改善了获得深度和持续分子反应(DMR,定义为稳定的 MR4 和 MR4.5)的慢性髓性白血病(CML)患者的总生存期(OS)。这些患者可能会尝试停止治疗。在我们的分析中,我们报告了在一大群 CP-CML 患者中,由于反应时间和作为一线治疗的不同 TKI 而导致的资格标准差异:数据由 GIMEMA 于 2014 年建立的网络 LabNet CML 导出。该网络对分布在意大利各地的51个实验室的分子诊断和分子残留病(MRD)监测方法进行了标准化和统一:在分析的1777名患者中,有774人拥有所有可评估的时间点(3个月、6个月和12个月)。3个月时,有40名患者≥MR4:其中伊马替尼14人(3.6%)、达沙替尼8人(5.8%)、尼洛替尼18人(7.4%)(P = .093);6个月时,146名患者MR4:伊马替尼42人(11%)、达沙替尼38人(28%)、尼洛替尼66人(27%)(P < .001)。12个月后,231名患者达到了DMR:伊马替尼为85人(22%),达沙替尼为55人(40%),尼洛替尼为91人(38%)(P < .001)。在3个月时至少达到≥MR2可预测任何观察时间点的DMR:使用伊马替尼时,67%的患者在2年内达到≥MR2,而使用达沙替尼时,30%的患者在2年内达到≥MR2,这在3个月时达到≥MR2的患者中意义重大(18%的患者在2年内达到≥MR2,而使用尼洛替尼时,9.9%的患者在2年内达到≥MR2):总之,3 个月时≥MR2 和 MR3 似乎可预测任何时间点的 DMR。考虑到停药的先决条件是持续的 DMR,只有少数患者有资格停药,无论接受的是哪种前线治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Deep Molecular Response Rate in Chronic Phase Chronic Myeloid Leukemia: Eligibility to Discontinuation Related to Time to Response and Different Frontline TKI in the Experience of the Gimema Labnet CML National Network.

Background: In the last decade, TKIs improved the overall survival (OS) of chronic myeloid leukemia (CML) patients who achieved a deep and sustained molecular response (DMR, defined as stable MR4 and MR4.5). Those patients may attempt therapy discontinuation. In our analysis, we report the differences in eligibility criteria due to time of response and different TKI used as frontline treatment analyzed in a large cohort of CP-CML patients.

Methods: Data were exported by LabNet CML, a network founded by GIMEMA in 2014. The network standardized and harmonized the molecular methodology among 51 laboratories distributed all over Italy for the diagnosis and molecular residual disease (MRD) monitoring.

Results: Out of 1777 patients analyzed, 774 had all evaluable timepoints (3, 6, and 12 months). At 3 months, 40 patients obtained ≥MR4: of them 14 (3.6%) with imatinib, 8 (5.8%) with dasatinib, and 18 (7.4%) with nilotinib (P = .093); at 6 months, 146 patients were in MR4: 42 (11%) with imatinib, 38 (28%) with dasatinib, and 66 (27%) with nilotinib (P < .001). At 12 months, 231 patients achieved a DMR: 85 (22%) with imatinib, 55 (40%) with dasatinib and 91 (38%) with nilotinib (P < .001). Achieving at least ≥MR2 at 3 months, was predictive of a DMR at any timepoint of observation: with imatinib 67% versus 30% of patients with 2 years was significant for patients who at 3 months had ≥MR2 (18% vs. 9.9% of pts with

Conclusion: In conclusion, reaching ≥MR2 and a MR3 at 3 months it seems predictive of a DMR at any time point. Considering the prerequisite for a discontinuation with a sustained DMR only a minority of patients can be eligible for the discontinuation, regardless the frontline treatment received.

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来源期刊
CiteScore
2.70
自引率
3.70%
发文量
1606
审稿时长
26 days
期刊介绍: Clinical Lymphoma, Myeloma & Leukemia is a peer-reviewed monthly journal that publishes original articles describing various aspects of clinical and translational research of lymphoma, myeloma and leukemia. Clinical Lymphoma, Myeloma & Leukemia is devoted to articles on detection, diagnosis, prevention, and treatment of lymphoma, myeloma, leukemia and related disorders including macroglobulinemia, amyloidosis, and plasma-cell dyscrasias. The main emphasis is on recent scientific developments in all areas related to lymphoma, myeloma and leukemia. Specific areas of interest include clinical research and mechanistic approaches; drug sensitivity and resistance; gene and antisense therapy; pathology, markers, and prognostic indicators; chemoprevention strategies; multimodality therapy; and integration of various approaches.
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