A Somatic Mutation in Moesin Drives Progression into Acute Myeloid Leukemia

Overview

Journal Sci Adv

Specialties Biology
Science

Date 2022 Apr 20

PMID 35442741

Authors

Ouyang Yuan

Amol Ugale

Tommaso De Marchi

Vimala Anthonydhason

Anna Konturek-Ciesla

Haixia Wan

Mohamed Eldeeb

Caroline Drabe

Maria Jassinskaja

Jenny Hansson

Isabel Hidalgo

Talia Velasco-Hernandez

Jorg Cammenga

Jeffrey A Magee

Emma Nimeus

David Bryder

Affiliations

Soon will be listed here.

Abstract

Acute myeloid leukemia (AML) arises when leukemia-initiating cells, defined by a primary genetic lesion, acquire subsequent molecular changes whose cumulative effects bypass tumor suppression. The changes that underlie AML pathogenesis not only provide insights into the biology of transformation but also reveal novel therapeutic opportunities. However, backtracking these events in transformed human AML samples is challenging, if at all possible. Here, we approached this question using a murine in vivo model with an MLL-ENL fusion protein as a primary molecular event. Upon clonal transformation, we identified and extensively verified a recurrent codon-changing mutation (ArgCys) in the ERM protein moesin that markedly accelerated leukemogenesis. Human cancer-associated moesin mutations at the conserved arginine-295 residue similarly enhanced MLL-ENL-driven leukemogenesis. Mechanistically, the mutation interrupted the stability of moesin and conferred a neomorphic activity to the protein, which converged on enhanced extracellular signal-regulated kinase activity. Thereby, our studies demonstrate a critical role of ERM proteins in AML, with implications also for human cancer.

Citing Articles

DNMT3A mutation promotes leukemia development through NAM-NAD metabolic reprogramming.

Yang X, Wang X, Yang Y, Li Z, Chen Y, Shang S J Transl Med. 2023; 21(1):481.

PMID: 37464424 PMC: 10355022. DOI: 10.1186/s12967-023-04323-z.

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