Next‐generation sequencing reveals the presence of  DDX41  mutations in acute lymphoblastic leukemia and aplastic anemia | Zendy

Zhang Yang | Zendy; Wang Fang | Zendy; Chen Xue | Zendy; Liu Hong | Zendy; Wang Xiaoliang | Zendy; Chen Jiaqi | Zendy; Cao Panxiang | Zendy; Ma Xiaoli | Zendy; Liu Hongxing | Zendy

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Next‐generation sequencing reveals the presence of DDX41 mutations in acute lymphoblastic leukemia and aplastic anemia

Author(s) -

Zhang Yang,

Wang Fang,

Chen Xue,

Liu Hong,

Wang Xiaoliang,

Chen Jiaqi,

Cao Panxiang,

Ma Xiaoli,

Liu Hongxing

Publication year - 2021

Publication title -

ejhaem

Language(s) - English

Resource type - Journals

ISSN - 2688-6146

DOI - 10.1002/jha2.256

Subject(s) - lymphoblastic leukemia , aplastic anemia , medicine , cancer research , mutation , dna sequencing , leukemia , genetics , biology , immunology , gene , bone marrow

Limited studies have been described DEAD‐box helicase 41 ( DDX41) mutations in hematological diseases other than myeloid neoplasms. In this study, DDX41 mutations were identified in 0.8% of myeloid neoplasms, 0.9% of acute lymphoblastic leukemia (ALL), and 1.0% of aplastic anemia (AA). A total of 15 causal DDX41 variants in 14 patients were detected; seven of which have not been reported previously. In myeloid neoplasms, the median age of patients with germline missense was lower than that of germline nonsense mutations. In ALL, the characteristics of DDX41 mutation were distinct. This study first reported DDX41 mutations in ALL and AA, expanding its mutation and phenotypic spectrum.

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