H3K79me2/3 controls enhancer-promoter interactions and activation of the pan-cancer stem cell marker PROM1/CD133 in MLL-AF4 leukemia cells
Godfrey, L. (University of Oxford. Department of Medicine)
Crump, N. T. (University of Oxford. Department of Medicine)
O'Byrne, Sorcha (Department of Paediatrics. University of Oxford)
Lau, I. J. (University of Oxford. Department of Medicine)
Rice, S. (University of Oxford. Department of Medicine)
Harman, J. R. (University of Oxford. Department of Medicine)
Jackson, T. (Department of Paediatrics. University of Oxford)
Elliott, N. (Department of Paediatrics. University of Oxford)
Buck, G. (Department of Paediatrics. University of Oxford)
Connor, C. (Great Ormond Street Hospital for Children (Londres))
Thorne, R. (University of Oxford. Department of Medicine)
Knapp, D. J. H. F. (MRC Weatherall Institute of Molecular Medicine. Radcliffe Department of Medicine. University of Oxford)
Heidenreich, O. (Newcastle University. Wolfson Childhood Cancer Research Centre)
Vyas, P. (Department of Haematology. Oxford University Hospitals NHS Foundation Trust)
Menéndez Bujan, Pablo (Institut Germans Trias i Pujol. Institut de Recerca contra la Leucèmia Josep Carreras)
Inglott, S. (Great Ormond Street Hospital for Children (Londres))
Ancliff, P. (Great Ormond Street Hospital for Children (Londres))
Geng, H. (Department of Laboratory Medicine. University of California. San Francisco)
Roberts, I. (Department of Paediatrics. University of Oxford)
Roy, A. (Department of Paediatrics. University of Oxford)
Milne, T. A. (University of Oxford. Department of Medicine)
Universitat Autònoma de Barcelona

Data:	2021
Resum:	MLL gene rearrangements (MLLr) are a common cause of aggressive, incurable acute lymphoblastic leukemias (ALL) in infants and children, most of which originate in utero. The most common MLLr produces an MLL-AF4 fusion protein. MLL-AF4 promotes leukemogenesis by activating key target genes, mainly through recruitment of DOT1L and increased histone H3 lysine-79 methylation (H3K79me2/3). One key MLL-AF4 target gene is PROM1, which encodes CD133 (Prominin-1). CD133 is a pentaspan transmembrane glycoprotein that represents a potential pan-cancer target as it is found on multiple cancer stem cells. Here we demonstrate that aberrant PROM1/CD133 expression is essential for leukemic cell growth, mediated by direct binding of MLL-AF4. Activation is controlled by an intragenic H3K79me2/3 enhancer element (KEE) leading to increased enhancer-promoter interactions between PROM1 and the nearby gene TAPT1. This dual locus regulation is reflected in a strong correlation of expression in leukemia. We find that in PROM1/CD133 non-expressing cells, the PROM1 locus is repressed by polycomb repressive complex 2 (PRC2) binding, associated with reduced expression of TAPT1, partially due to loss of interactions with the PROM1 locus. Together, these results provide the first detailed analysis of PROM1/CD133 regulation that explains CD133 expression in MLLr ALL.
Ajuts:	European Commission CoG-2014-646903 Ministerio de Economía y Competitividad SAF2016-80481-R
Nota:	Altres ajuts: Acknowledgements TAM, LG, NTC, I-JL, RT, JRH, and SR were funded by Medical Research Council (MRC, UK) Molecular Haematology Unit grant MC_UU_12009/6, MC_UU_00016/6, and MR/ M003221/1. AR was supported by a Bloodwise Clinician Scientist Fellowship (grants: 14041 and 17001), Wellcome Trust Clinical Research Career Development Fellowship (216632/Z/19/Z), Lady Tata Memorial International Fellowship, and EHA-ASH Translational Research Training in Hematology Fellowship. SOB was funded by the Department of Paediatrics and Alexander Thatte Fund, University of Oxford. DJHFK is funded by a CIHR Postdoctoral Fellowship. IR is supported by the NIHR Oxford BRC, by a Bloodwise Program Grant (13001) and by the MRC Molecular Haematology Unit (MC_UU_12009/14). PV via the Molecular Haematology Unit (MC_UU_12009) and the National Institute for Health Research (NIHR) Oxford Biomedical Research Centre (BRC) Programme. We would like to acknowledge the WIMM Flow Cytometry Facility which is supported by the MRC HIU, MRC MHU (MC_UU_12009), NIHR Oxford BRC, Kay Kendall Leukemia Fund (KKL1057), John Fell Fund (131/030 and 101/517), the EPA fund (CF182 and CF170), and by the WIMM Strategic Alliance awards G0902418 and MC_UU_12025. We thank the High-Throughput Genomics Group at the Wellcome Trust Centre for Human Genetics (funded by Wellcome Trust Grant Reference 090532/Z/09/Z); the MRC WIMM Centre for Computational Biology (CCB), Radcliffe Department of Medicine, University of Oxford; and Jelena Telenius for the use of her pipelines. B-ALL work in PM's lab is financially supported by [...], the Fundación Uno entre Cienmil, the Fundación Leo Messi. PM also acknowledges structural support from the Obra Social La Caixa-Fundaciò Josep Carreras. The human fetal material was provided by the Joint MRC/ Wellcome Trust Grant 099175/Z/ 12/Z Human Developmental Biology Resource (http://hdbr.org). We gratefully acknowledge the kind generosity of patients, their parents, and staff at Great Ormond Street Hospital, London.
Drets:	Aquest document està subjecte a una llicència d'ús Creative Commons. Es permet la reproducció total o parcial, la distribució, la comunicació pública de l'obra i la creació d'obres derivades, fins i tot amb finalitats comercials, sempre i quan es reconegui l'autoria de l'obra original.
Llengua:	Anglès
Document:	Article ; recerca ; Versió publicada
Matèria:	Acute lymphocytic leukaemia ; Cancer genomics
Publicat a:	Leukemia, Vol. 35 Núm. 1 (january 2021) , p. 90-106, ISSN 1476-5551

DOI: 10.1038/s41375-020-0808-y
PMID: 32242051

17 p, 2.3 MB

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