Disease characteristics and outcomes of acute myeloid leukemia in germline RUNX1 deficiency (Familial Platelet Disorder with associated Myeloid Malignancy)

IF 7.6 2区医学 Q1 HEMATOLOGY

HemaSphere Pub Date : 2025-01-16 DOI:10.1002/hem3.70057

Martijn P. T. Ernst, Jurjen Versluis, Peter J. M. Valk, Marc Bierings, Rienk Y. J. Tamminga, Louise H. Hooimeijer, Konstanze Döhner, Paolo Gresele, Kiran Tawana, Saskia M. C. Langemeijer, Bert A. Van der Reijden, Helena Podgornik, Matjaz Sever, Tor H. A. Tvedt, Tom Vulliamy, Jude Fitzgibbon, Inderjeet Dokal, Panagiotis Baliakas, José M. Bastida, Christian Pohlkamp, Torsten Haferlach, Lise Larcher, Jean Soulier, Roger E. G. Schutgens, Kathleen Freson, Nicolas Duployez, Bob Löwenberg, Katrin Ericson, Jörg Cammenga, Tim Ripperger, Marc H. G. P. Raaijmakers

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Abstract

Familial Platelet Disorder with associated Myeloid Malignancy (FPDMM, FPD/AML, RUNX1-FPD), caused by monoallelic deleterious germline RUNX1 variants, is characterized by bleeding diathesis and predisposition for hematologic malignancies, particularly myelodysplastic syndrome (MDS) and acute myeloid leukemia (AML). Clinical data on FPDMM-associated AML (FPDMM-AML) are limited, complicating evidence-based clinical decision-making. Here, we present retrospective genetic and clinical data of the largest cohort of FPDMM patients reported to date. We describe 159 European patients (from 94 families) of whom 134 were evaluable for the development of malignant disease. Sixty developed a hematologic malignancy (44.8%), most frequently AML (36/134, 26.9%) or MDS (18/134, 13.4%). Somatic alterations of RUNX1 by gene mutation (48%) and chromosome 21 aberrations (14.3%) were the most common somatic genetic aberrations in FPDMM-AML, followed by FLT3-ITD mutations (24.1%). Somatic RUNX1 and FLT3-ITD mutations were not detected in FPDMM-associated MDS, suggesting important contributions to leukemic transformation. Remission-induction chemotherapy resulted in complete remission in 80% of FPDMM-AML patients with a 5-year overall survival (OS) of 50.4%. Survival outcome was non-inferior compared to a large cohort of newly diagnosed adult RUNX1-mutated AML (5-year OS 36.6%, p = 0.5), with relatively infrequent concurrent adverse risk somatic aberrations (ASXL1 mutation, monosomal karyotype, monosomy 5/del 5q) in FPDMM-AML. Collectively, data support the notion that step-wise leukemic evolution in FPDMM is associated with distinct genetic events and indicate that a substantial subset of FPDMM-AML patients achieves prolonged survival with conventional AML treatment, including allogeneic stem cell transplant. These findings are anticipated to inform personalized clinical decision-making in this rare disorder.

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种系RUNX1缺乏症（家族性血小板紊乱伴髓系恶性肿瘤）患者急性髓系白血病的疾病特征和预后

家族性血小板紊乱伴髓系恶性肿瘤（FPDMM, FPD/AML, RUNX1-FPD）是由单等位基因有害种系RUNX1变异引起的，其特征是出血和血液系统恶性肿瘤易感性，特别是骨髓增生异常综合征（MDS）和急性髓系白血病（AML）。fpdmm相关AML （FPDMM-AML）的临床数据有限，使循证临床决策复杂化。在这里，我们提出了迄今为止报道的最大FPDMM患者队列的回顾性遗传和临床数据。我们描述了159名欧洲患者（来自94个家庭），其中134人可评估恶性疾病的发展。60例发生血液学恶性肿瘤（44.8%），最常见的是AML（36/134, 26.9%）或MDS（18/134, 13.4%）。FPDMM-AML中最常见的体细胞遗传畸变是RUNX1基因突变（48%）和21号染色体畸变（14.3%），其次是FLT3-ITD突变（24.1%）。在fpdmm相关的MDS中未检测到体细胞RUNX1和FLT3-ITD突变，提示在白血病转化中起重要作用。缓解诱导化疗导致80%的FPDMM-AML患者完全缓解，5年总生存率（OS）为50.4%。与新诊断的成人runx1突变AML的大队列相比，生存结果并不差（5年生存率36.6%,p = 0.5）， FPDMM-AML中并发不良风险体细胞畸变（ASXL1突变，单染色体核型，单体5/del 5q）相对较少。总的来说，数据支持FPDMM的逐步白血病进化与不同的遗传事件相关的观点，并表明FPDMM-AML患者的相当一部分通过传统的AML治疗（包括同种异体干细胞移植）延长了生存期。这些发现有望为这种罕见疾病的个性化临床决策提供信息。

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来源期刊

HemaSphere Medicine-Hematology

CiteScore

6.10

自引率

4.50%

发文量

2776

审稿时长

7 weeks

期刊介绍： HemaSphere, as a publication, is dedicated to disseminating the outcomes of profoundly pertinent basic, translational, and clinical research endeavors within the field of hematology. The journal actively seeks robust studies that unveil novel discoveries with significant ramifications for hematology. In addition to original research, HemaSphere features review articles and guideline articles that furnish lucid synopses and discussions of emerging developments, along with recommendations for patient care. Positioned as the foremost resource in hematology, HemaSphere augments its offerings with specialized sections like HemaTopics and HemaPolicy. These segments engender insightful dialogues covering a spectrum of hematology-related topics, including digestible summaries of pivotal articles, updates on new therapies, deliberations on European policy matters, and other noteworthy news items within the field. Steering the course of HemaSphere are Editor in Chief Jan Cools and Deputy Editor in Chief Claire Harrison, alongside the guidance of an esteemed Editorial Board comprising international luminaries in both research and clinical realms, each representing diverse areas of hematologic expertise.