HOXBLINC long non-coding RNA activation promotes leukemogenesis in NPM1-mutant acute myeloid leukemia

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作者
Ganqian Zhu
Huacheng Luo
Yang Feng
Olga A. Guryanova
Jianfeng Xu
Shi Chen
Qian Lai
Arati Sharma
Bing Xu
Zhigang Zhao
Ru Feng
Hongyu Ni
David Claxton
Ying Guo
Ruben A. Mesa
Yi Qiu
Feng-Chun Yang
Wei Li
Stephen D. Nimer
Suming Huang
Mingjiang Xu
机构
[1] University of Texas Health San Antonio,Department of Molecular Medicine
[2] University of Miami Miller School of Medicine,Department of Biochemistry and Molecular Biology
[3] Pennsylvania State University College of Medicine,Department of Pediatrics
[4] University of Florida College of Medicine,Department of Pharmacology and Therapeutics
[5] Dan L. Duncan Cancer Center,Department of Molecular and Cellular Biology
[6] Baylor College of Medicine,Division of Hematology/Oncology, Department of Medicine
[7] Pennsylvania State University College of Medicine,Department of Hematology
[8] The First Affiliated Hospital of Xiamen University,Department of Hematology and Oncology
[9] Tianjin Medical University Cancer Institute and Hospital,Department of Hematology, Nanfang Hospital
[10] National Clinical Research Center for Cancer,Department of Pathology
[11] Key Laboratory of Cancer Prevention and Therapy,Penn State Cancer Institute
[12] Southern Medical University,Department of Cell System & Anatomy
[13] Wayne State University School of Medicine,Department of Medicine
[14] Pennsylvania State University College of Medicine,Mays Cancer Center
[15] University of Texas Health San Antonio,Department of Cellular & Molecular Physiology
[16] University of Texas Health San Antonio,Sylvester Comprehensive Cancer Center
[17] University of Texas Health San Antonio,Division of Computational Biomedicine, Department of Biological Chemistry, School of Medicine
[18] Pennsylvania State University College of Medicine,Department of Medicine
[19] University of Miami Miller School of Medicine,undefined
[20] University of California,undefined
[21] University of Miami Miller School of Medicine,undefined
来源
Nature Communications | / 12卷
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摘要
Nucleophosmin (NPM1) is the most commonly mutated gene in acute myeloid leukemia (AML) resulting in aberrant cytoplasmic translocation of the encoded nucleolar protein (NPM1c+). NPM1c+ maintains a unique leukemic gene expression program, characterized by activation of HOXA/B clusters and MEIS1 oncogene to facilitate leukemogenesis. However, the mechanisms by which NPM1c+ controls such gene expression patterns to promote leukemogenesis remain largely unknown. Here, we show that the activation of HOXBLINC, a HOXB locus-associated long non-coding RNA (lncRNA), is a critical downstream mediator of NPM1c+-associated leukemic transcription program and leukemogenesis. HOXBLINC loss attenuates NPM1c+-driven leukemogenesis by rectifying the signature of NPM1c+ leukemic transcription programs. Furthermore, overexpression of HoxBlinc (HoxBlincTg) in mice enhances HSC self-renewal and expands myelopoiesis, leading to the development of AML-like disease, reminiscent of the phenotypes seen in the Npm1 mutant knock-in (Npm1c/+) mice. HoxBlincTg and Npm1c/+ HSPCs share significantly overlapped transcriptome and chromatin structure. Mechanistically, HoxBlinc binds to the promoter regions of NPM1c+ signature genes to control their activation in HoxBlincTg HSPCs, via MLL1 recruitment and promoter H3K4me3 modification. Our study reveals that HOXBLINC lncRNA activation plays an essential oncogenic role in NPM1c+ leukemia. HOXBLINC and its partner MLL1 are potential therapeutic targets for NPM1c+ AML.
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