Novel Germ Line DDX41 Mutations Define Families with a Lower Age of MDS/AML Onset and Lymphoid Malignancies

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2015 Dec 30

PMID 26712909

Citations 102

Authors

Maya Lewinsohn

Anna L Brown

Luke M Weinel

Connie Phung

George Rafidi

Ming K Lee

Andreas W Schreiber

Jinghua Feng

Milena Babic

Chan-Eng Chong

Young Lee

Agnes Yong

Graeme K Suthers

Nicola Poplawski

Meryl Altree

Kerry Phillips

Louise Jaensch

Miriam Fine

Richard J DAndrea

Ian D Lewis

Bruno C Medeiros

Daniel A Pollyea

Mary-Claire King

Tom Walsh

Sioban Keel

Akiko Shimamura

Lucy A Godley

Christopher N Hahn

Jane E Churpek

Hamish S Scott

Affiliations

Soon will be listed here.

Abstract

Recently our group and others have identified DDX41 mutations both as germ line and acquired somatic mutations in families with multiple cases of late onset myelodysplastic syndrome (MDS) and/or acute myeloid leukemia (AML), suggesting that DDX41 acts as a tumor suppressor. To determine whether novel DDX41 mutations could be identified in families with additional types of hematologic malignancies, our group screened two cohorts of families with a diverse range of hematologic malignancy subtypes. Among 289 families, we identified nine (3%) with DDX41 mutations. As previously observed, MDS and AML were the most common malignancies, often of the erythroblastic subtype, and 1 family displayed early-onset follicular lymphoma. Five novel mutations were identified, including missense mutations within important functional domains and start-loss and splicing mutations predicted to result in truncated proteins. We also show that most asymptomatic mutation carriers have normal blood counts until malignancy develops. This study expands both the mutation and phenotypic spectra observed in families with germ line DDX41 mutations. With an increasing number of both inherited and acquired mutations in this gene being identified, further study of how DDX41 disruption leads to hematologic malignancies is critical.

Citing Articles

Germline DDX41 mutations in myeloid neoplasms: the current clinical and molecular understanding.

Kida J, Chlon T Curr Opin Hematol. 2024; 32(2):67-76.

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