Aberrant DNA hydroxymethylation reshapes transcription factor binding in myeloid neoplasms

Author:

Li Jia,Hong Tingting,Wei Yue,Guo Lei,Lee Minjung,Yang Hui,Class Caleb,Yang Yaling,Wang Xiaoqiong,He Hua,Siwko Stefan,You M. James,Zhou Yubin,Garcia-Manero Guillermo,Huang Yun

Abstract

AbstractEpigenetic abnormalities in DNA hydroxymethylation (5hmC) have been detected in patients with myeloid neoplasms, suggesting that 5hmC might act as a valuable epigenetic mark to reflect the disease status of myeloid neoplasms. Here, we report systematic genome-wide mapping of the DNA hydroxymethylomes in over 70 patients with myeloid neoplasms. Our integrative analysis leads to the identification of distinct 5hmC signatures that can sensitively discriminate patients from healthy individuals. At the molecular level, we unveiled dynamic 5hmC changes within key transcription factor (e.g., the CEBP family) binding motifs that are essential for hematopoiesis and myeloid lineage specification. 5hmC redistribution was found to alter the genome-wide binding of CEBP-α, thereby reprogramming transcriptional outputs to affect leukemia cell survival and stemness. Taken together, we provide a comprehensive 5hmC atlas representative of myeloid neoplasms, which sets the stage for future exploration on the epigenetic etiology of hematological malignancies. Mechanistically, our study further furnishes important insights into how abnormal 5hmC distribution in patients directly interrupts the binding of transcription factors to reshape transcriptional landscapes and aggravate leukemogenesis.

Funder

Cancer Prevention and Research Institute of Texas

Welch Foundation

National Institutes of Health

American Cancer Society

Publisher

Springer Science and Business Media LLC

Subject

Genetics (clinical),Developmental Biology,Genetics,Molecular Biology

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