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    Differentiation block in acute myeloid leukemia regulated by intronic sequences of FTO

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    Authors
    Camera, Francesco
    Romero-Camarero, Isabel
    Revell, Bradley H
    Amaral, Fabio M R
    Sinclair, Oliver J
    Simeoni, Fabrizio
    Wiseman, Daniel H.
    Stojic, L.
    Somervaille, Tim C P
    Affiliation
    Leukaemia Biology Laboratory, Cancer Research UK Manchester Institute, The University of Manchester, The Oglesby Cancer Research Centre Building, 555 Wilmslow Road, M20 4GJ Manchester, UK
    Issue Date
    2023
    
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    Abstract
    Iroquois transcription factor gene IRX3 is highly expressed in 20-30% of acute myeloid leukemia (AML) and contributes to the pathognomonic differentiation block. Intron 8 FTO sequences ∼220kB downstream of IRX3 exhibit histone acetylation, DNA methylation, and contacts with the IRX3 promoter, which correlate with IRX3 expression. Deletion of these intronic elements confirms a role in positively regulating IRX3. RNAseq revealed long non-coding (lnc) transcripts arising from this locus. FTO-lncAML knockdown (KD) induced differentiation of AML cells, loss of clonogenic activity, and reduced FTO intron 8:IRX3 promoter contacts. While both FTO-lncAML KD and IRX3 KD induced differentiation, FTO-lncAML but not IRX3 KD led to HOXA downregulation suggesting transcript activity in trans. FTO-lncAMLhigh AML samples expressed higher levels of HOXA and lower levels of differentiation genes. Thus, a regulatory module in FTO intron 8 consisting of clustered enhancer elements and a long non-coding RNA is active in human AML, impeding myeloid differentiation
    Citation
    Camera F, Romero-Camarero I, Revell BH, Amaral FMR, Sinclair OJ, Simeoni F, et al. Differentiation block in acute myeloid leukemia regulated by intronic sequences of FTO. iScience. 2023 Aug 18;26(8):107319. PubMed PMID: 37539037. Pubmed Central PMCID: PMC10393733. Epub 2023/08/04. eng.
    Journal
    iScience
    URI
    http://hdl.handle.net/10541/626491
    DOI
    10.1016/j.isci.2023.107319
    PubMed ID
    37539037
    Additional Links
    https://dx.doi.org/10.1016/j.isci.2023.107319
    Type
    Article
    Language
    en
    ae974a485f413a2113503eed53cd6c53
    10.1016/j.isci.2023.107319
    Scopus Count
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    All Paterson Institute for Cancer Research

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