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A non-canonical lymphoblast in refractory childhood T-cell leukaemia

  • Bram S.J. Lim
  • , Holly J. Whitfield
  • , Mi K. Trinh
  • , Gianna Bloye
  • , Rebecca Thomas
  • , Nathaniel D. Anderson
  • , Anna Wenger
  • , Angus Hodder
  • , Taryn D. Treger
  • , Henry Lee-Six
  • , Tim H.H. Coorens
  • , Conor Parks
  • , Toochi Ogbonnah
  • , Petri Pölönen
  • , Charles G. Mullighan
  • , David T. Teachey
  • , Jason Xu
  • , Kai Tan
  • , Melanie Hagleitner
  • , Lennart Kester
  • Frank N. van Leeuwen, Gordon Beattie, Marc R. Mansour, Owen Williams, Jack Bartram, Stuart Adams, Laura Jardine, Sam Behjati, David O’Connor

Onderzoeksoutput: Bijdrage aan tijdschriftArtikelpeer review

Samenvatting

Refractory cancers may arise either through the acquisition of resistance mechanisms or represent distinct disease states. The origin of childhood T-cell acute lymphoblastic leukaemia (T-ALL) that does not respond to initial treatment, i.e. refractory disease, is unknown. Refractory T-ALL carries a poor prognosis and cannot be predicted at diagnosis. Here, we perform single cell mRNA sequencing of T-ALL from 58 children (84 samples) who did, or did not respond to initial treatment. We identify a transcriptionally distinctive blast population, exhibiting features of innate-like lymphocytes, as the major source of refractory disease. Evidence of such blasts at diagnosis heralds refractory disease across independent datasets and is associated with survival in a large, contemporary trial cohort. Our findings portray refractory T-ALL as a distinct disease with the potential for immediate clinical utility.

Originele taal-2Engels
Artikelnummer9397
TijdschriftNature communications
Volume16
Nummer van het tijdschrift1
DOI's
StatusGepubliceerd - 12 nov. 2025

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