Open Access
Open access
Proceedings of the National Academy of Sciences of the United States of America, volume 114, issue 20, pages 5237-5242

Conditional knockin of Dnmt3a R878H initiates acute myeloid leukemia with mTOR pathway involvement

Yu Jun Dai 1
Yue-Ying Wang 1
Jin Yan Huang 1
Xia Li 1
Shi-xiao Dong 1
Jie Xu 1
Jing Lu 1
Xian Bin Su 2
Ying Yang 1
Wei-Na Zhang 1
Pan-Pan Wang 1
Song Fang Wu 1
Ting Huang 1
Jian-Qing Mi 1
Ze‐Guang Han 2
Zhu Chen 1, 2
Sai-juan CHEN 1, 2
Show full list: 17 authors
Publication typeJournal Article
Publication date2017-05-11
scimago Q1
SJR3.737
CiteScore19.0
Impact factor9.4
ISSN00278424, 10916490
Multidisciplinary
Abstract
Significance

DNMT3A is a critical epigenetic modifier and tumor suppressor in the hematopoietic system. This gene is frequently mutated in hematopoietic malignancies, including acute myeloid leukemia (AML), with Dnmt3a R878H being the most common mutant. By using a conditional knockin approach, this study shows that Dnmt3a R878H is sufficient to initiate AML and recapitulate human leukemic features in mice. The leukemia-initiating cells are enriched in hematopoietic stem/progenitor cells. Through gene expression profiling, DNA methylation and histone modification analysis, and functional tests on important regulators for cell proliferation and differentiation in an animal model, this study has not only discovered mTOR pathway activation as a key player in the disease mechanism but also revealed the potential therapeutic effects of mTOR inhibition on DNMT3A mutation-related leukemia.

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