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AML with germline DDX41 variants is a clinicopathologically distinct entity with an indolent clinical course and favorable outcome

Authors :
Peng, Li
Thomas, White
Wei, Xie
Wei, Cui
Deniz, Peker
Gang, Zeng
Huan-You, Wang
Jennie, Vagher
Sara, Brown
Margaret, Williams
Tibor, Kovacsovics
Jay L, Patel
Source :
Leukemia. 36(3)
Publication Year :
2021

Abstract

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.

Details

ISSN :
14765551
Volume :
36
Issue :
3
Database :
OpenAIRE
Journal :
Leukemia
Accession number :
edsair.pmid..........237fd82333b9454cd573426e1c53d4f0