Blood Cancer Journal (Nov 2021)

Cancer drivers and clonal dynamics in acute lymphoblastic leukaemia subtypes

  • James B. Studd,
  • Alex J. Cornish,
  • Phuc H. Hoang,
  • Philip Law,
  • Ben Kinnersley,
  • Richard Houlston

DOI
https://doi.org/10.1038/s41408-021-00570-9
Journal volume & issue
Vol. 11, no. 11
pp. 1 – 10

Abstract

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Abstract To obtain a comprehensive picture of composite genetic driver events and clonal dynamics in subtypes of paediatric acute lymphoblastic leukaemia (ALL) we analysed tumour-normal whole genome sequencing and expression data from 361 newly diagnosed patients. We report the identification of both structural drivers, as well as recurrent non-coding variation in promoters. Additionally we found the transcriptional profile of histone gene cluster 1 and CTCF altered tumours shared hallmarks of hyperdiploid ALL suggesting a ‘hyperdiploid like’ subtype. ALL subtypes are driven by distinct mutational processes with AID mutagenesis being confined to ETV6-RUNX1 tumours. Subclonality is a ubiquitous feature of ALL, consistent with Darwinian evolution driving selection and expansion of tumours. Driver mutations in B-cell developmental genes (IKZF1, PAX5, ZEB2) tend to be clonal and RAS/RTK mutations subclonal. In addition to identifying new avenues for therapeutic exploitation, this analysis highlights that targeted therapies should take into account composite mutational profile and clonality.