Division of Hematopathology, Department of Pathology, University of Utah Health, Salt Lake City, UT, USA.
Genomics Laboratory, ARUP Laboratories, Salt Lake City, UT, USA.
Leukemia. 2022 Mar;36(3):664-674. doi: 10.1038/s41375-021-01404-0. Epub 2021 Oct 20.
Germline DDX41 variants in myeloid neoplasms (MNs) are not uncommon, and we explored the prevalence and characterized the clinical and pathologic features in a cohort of 3132 unrelated adult MN patients. By targeted next-generation sequencing, we identified 28 patients (20 men and 8 women) with pathogenic germline DDX41 variants who developed acute myeloid leukemia (AML), in which only 3 (11%) had a family history (FH) of MNs. A subacute clinical course of cytopenia (mean duration of 11.2 months, range 0-72 months) prior to the initial AML diagnosis was accompanied by a low blast count (median at 30%, range 20-70%) in hypocellular marrows (93% of all patients), in vast contrast to the typical proliferative subtypes of AML in the elderly. Most patients had a normal karyotype (75%) and acquired a second DDX41 variant (69%). A favorable overall survival (OS) was observed in comparison to that of common subtypes of AML with wild-type DDX41 in age-matched patients. Our study demonstrated that the frequent germline pathogenic DDX41 variants characterized a clinically distinct AML entity. Features characteristic of DDX41-mutated AML include male predominance, often lack of FH, indolent course, low proliferative potential, frequent somatic DDX41 variants, and a favorable OS.
胚系 DDX41 变异在髓系肿瘤(MNs)中并不罕见,我们在 3132 名无关的成年 MN 患者队列中探索了其患病率,并对其临床和病理特征进行了特征分析。通过靶向下一代测序,我们确定了 28 名(20 名男性和 8 名女性)患有致病性胚系 DDX41 变异的患者发生了急性髓系白血病(AML),其中只有 3 名(11%)有 MNs 的家族史(FH)。在初始 AML 诊断前,血细胞减少症的亚急性临床病程(平均持续时间为 11.2 个月,范围为 0-72 个月)伴有低原始细胞计数(中位数为 30%,范围为 20-70%)在低细胞性骨髓中(所有患者的 93%),与老年人中典型的 AML 增殖亚型形成鲜明对比。大多数患者具有正常核型(75%)和获得第二种 DDX41 变异(69%)。与年龄匹配的 DDX41 野生型 AML 常见亚型相比,观察到了较好的总生存(OS)。我们的研究表明,频繁的胚系致病性 DDX41 变异特征是一种具有独特临床特征的 AML 实体。DDX41 突变 AML 的特征性特征包括男性为主、通常缺乏 FH、惰性病程、低增殖潜能、频繁的体细胞 DDX41 变异和较好的 OS。
