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A human fetal liver-derived infant MLL-AF4 acute lymphoblastic leukemia model reveals a distinct fetal gene expression program

Author

Listed:
  • Siobhan Rice

    (University of Oxford)

  • Thomas Jackson

    (University of Oxford)

  • Nicholas T. Crump

    (University of Oxford)

  • Nicholas Fordham

    (University of Oxford)

  • Natalina Elliott

    (University of Oxford)

  • Sorcha O’Byrne

    (University of Oxford)

  • Maria del Mar Lara Fanego

    (Great Ormond Street Hospital for Children)

  • Dilys Addy

    (Great Ormond Street Hospital for Children)

  • Trisevgeni Crabb

    (Great Ormond Street Hospital for Children)

  • Carryl Dryden

    (Great Ormond Street Hospital for Children)

  • Sarah Inglott

    (Great Ormond Street Hospital for Children)

  • Dariusz Ladon

    (Great Ormond Street Hospital for Children)

  • Gary Wright

    (Great Ormond Street Hospital for Children)

  • Jack Bartram

    (Great Ormond Street Hospital for Children)

  • Philip Ancliff

    (Great Ormond Street Hospital for Children)

  • Adam J. Mead

    (University of Oxford)

  • Christina Halsey

    (University of Glasgow
    Royal Hospital for Children)

  • Irene Roberts

    (University of Oxford
    University of Oxford)

  • Thomas A. Milne

    (University of Oxford)

  • Anindita Roy

    (University of Oxford
    University of Oxford)

Abstract

Although 90% of children with acute lymphoblastic leukemia (ALL) are now cured, the prognosis for infant-ALL remains dismal. Infant-ALL is usually caused by a single genetic hit that arises in utero: an MLL/KMT2A gene rearrangement (MLL-r). This is sufficient to induce a uniquely aggressive and treatment-refractory leukemia compared to older children. The reasons for disparate outcomes in patients of different ages with identical driver mutations are unknown. Using the most common MLL-r in infant-ALL, MLL-AF4, as a disease model, we show that fetal-specific gene expression programs are maintained in MLL-AF4 infant-ALL but not in MLL-AF4 childhood-ALL. We use CRISPR-Cas9 gene editing of primary human fetal liver hematopoietic cells to produce a t(4;11)/MLL-AF4 translocation, which replicates the clinical features of infant-ALL and drives infant-ALL-specific and fetal-specific gene expression programs. These data support the hypothesis that fetal-specific gene expression programs cooperate with MLL-AF4 to initiate and maintain the distinct biology of infant-ALL.

Suggested Citation

  • Siobhan Rice & Thomas Jackson & Nicholas T. Crump & Nicholas Fordham & Natalina Elliott & Sorcha O’Byrne & Maria del Mar Lara Fanego & Dilys Addy & Trisevgeni Crabb & Carryl Dryden & Sarah Inglott & D, 2021. "A human fetal liver-derived infant MLL-AF4 acute lymphoblastic leukemia model reveals a distinct fetal gene expression program," Nature Communications, Nature, vol. 12(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-021-27270-z
    DOI: 10.1038/s41467-021-27270-z
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    References listed on IDEAS

    as
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    2. R. Torres & M. C. Martin & A. Garcia & Juan C. Cigudosa & J. C. Ramirez & S. Rodriguez-Perales, 2014. "Engineering human tumour-associated chromosomal translocations with the RNA-guided CRISPR–Cas9 system," Nature Communications, Nature, vol. 5(1), pages 1-8, September.
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