Mutant NPM1 Hijacks Transcriptional Hubs to Maintain Pathogenic Gene Programs in Acute Myeloid Leukemia
Abstract
Nucleophosmin (NPM1) is a ubiquitously expressed nucleolar protein with a wide range of biological functions. In 30% of acute myeloid leukemia (AML), the terminal exon of NPM1 is often found mutated, resulting in the addition of a nuclear export signal and a shift of the protein to the cytoplasm (NPM1c). AMLs carrying this mutation have aberrant expression of the HOXA/B genes, whose overexpression leads to leukemogenic transformation. Here, for the first time, we comprehensively prove that NPM1c binds to a subset of active gene promoters in NPM1c AMLs, including well-known leukemia-driving genes—HOXA/B cluster genes and MEIS1. NPM1c sustains the active transcription of key target genes by orchestrating a transcription hub and maintains the active chromatin landscape by inhibiting the activity of histone deacetylases. Together, these findings reveal the neomorphic function of NPM1c as a transcriptional amplifier for leukemic gene expression and open up new paradigms for therapeutic intervention. Significance: NPM1 mutation is the most common mutation in AML, yet the mechanism of how the mutant protein results in AML remains unclear. Here, for the first time, we prove mutant NPM1 directly binds to active chromatin regions and hijacks the transcription of AML-driving genes.
Additional Information
© 2022 The Authors; Published by the American Association for Cancer Research. This open access article is distributed under the Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0) license. We thank Dr. Margaret Goodell for her support of this work by sharing the OCI-AML3 NPM1c degron 2 cell line. We also thank Dr. Michael Gundry and Dr. Lorenzo Brunetti for their valuable suggestions during the discussion at the early phase of this project. We thank Dr. Chao Lu, Dr. Jia Fei, and Dr. Tianpeng Gu for their vibrant discussion on this project. We also thank Yushuai Liu and Shan Tang for their support on microscopy imaging and immunofluorescence. X. Zhang was supported by an American Society of Hematology Fellow Award and an EvansMDS research foundation Young Investigator Award during the execution of the project. T. Cierpicki is supported by the NIH/NCI (R01CA207272 and R01CA240514). J. Grembecka is supported by NIH/NCI (R01CA160467). L. Wan is supported by an NIH Director's New Innovator Award (1DP2HG012443), an NIH Pathway to Independence Award (R00CA226399), the Pew-Stewart Scholars Program for Cancer Research, a V Foundation Scholar Award, and an American Society of Hematology Scholar Award. Y. Liu is supported by an Abramson Family Cancer Research Institute Postdoctoral Fellowship. S. Chong is supported by a Shurl and Kay Curci Foundation Research Grant, the Pew-Stewart Scholars Program for Cancer Research (00036068), the Searle Scholars Program (SSP-2022-108), and a Merkin Innovation Seed Grant. Authors' Contributions. X.Q.D. Wang: Conceptualization, data curation, validation, investigation, visualization, methodology, writing–original draft, project administration. D. Fan: Data curation, formal analysis, investigation. Q. Han: Data curation, software, formal analysis. Y. Liu: Investigation. H. Miao: Investigation. X. Wang: Data curation, visualization. Q. Li: Data curation. D. Chen: Investigation. H. Gore: Investigation, methodology. P. Himadewi: Data curation. G.P. Pfeifer: Writing–review and editing. T. Cierpicki: Resources, supervision. J. Grembecka: Resources, supervision. J. Su: Data curation, software, supervision, writing–original draft, project administration. S. Chong: Data curation, supervision, visualization, writing–original draft, writing–review and editing. L. Wan: Supervision, writing–original draft, project administration, writing–review and editing. X. Zhang: Conceptualization, data curation, formal analysis, supervision, funding acquisition, investigation, visualization, methodology, writing–original draft, project administration, writing–review and editing. Authors' Disclosures. T. Cierpicki reports other support from Kura Oncology during the conduct of the study; grants and other support from the NIH outside the submitted work; and a patent for 16/082,645 issued, licensed, and with royalties paid from Kura Oncology. J. Grembecka reports other support from Kura Oncology and grants from the NIH (1R01CA160467 and 1R01CA201204) during the conduct of the study, as well as a patent for 16/082,645 issued, licensed, and with royalties paid from Kura Oncology. S. Chong reports grants from the Shurl and Kay Curci Foundation, The Pew Charitable Trusts, the Kinship Foundation, and the Merkin Institute for Translational Research during the conduct of the study. L. Wan reports serving as a consultant for Bridge Medicines. X. Zhang reports grants from the American Society of Hematology and EvansMDS research foundation during the conduct of the study. No disclosures were reported by the other authors. Data Availability. All CUT&RUN, ChIP-seq, RNA-seq, and Bru-seq data have been deposited to the Gene Expression Omnibus under accession GSE197387 (https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE197387).Attached Files
Published - 724.pdf
Supplemental Material - cd-22-0424_supplementary_figure_s1-s8_suppsf1.docx
Supplemental Material - cd-22-0424_supplementary_table_s1_suppst1.xlsx
Supplemental Material - cd-22-0424_supplementary_table_s2_suppst2.xlsx
Supplemental Material - cd-22-0424_supplementary_table_s3_suppst3.xlsx
Supplemental Material - cd-22-0424_supplementary_table_s4_suppst4.xlsx
Supplemental Material - cd-22-0424_supplementary_table_s5_suppst5.xlsx
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Additional details
- Alternative title
- Pathogenic Gene Programs in Acute Myeloid Leukemia
- PMCID
- PMC9975662
- Eprint ID
- 120318
- Resolver ID
- CaltechAUTHORS:20230322-270078000.2
- American Society of Hematology
- Edward P. Evans Foundation
- R01CA207272
- NIH
- R01CA240514
- NIH
- R01CA160467
- NIH
- 1DP2HG012443
- NIH
- R00CA226399
- NIH
- V Foundation for Cancer Research
- Abramson Family Cancer Research Institute
- Shurl and Kay Curci Foundation
- 00036068
- Pew Charitable Trusts
- SSP-2022-108
- Searle Scholars Program
- Caltech Merkin Institute for Translational Research
- Created
-
2023-03-22Created from EPrint's datestamp field
- Updated
-
2023-10-09Created from EPrint's last_modified field
- Caltech groups
- Richard N. Merkin Institute for Translational Research