Efficacy of third-party chimeric antigen receptor modified peripheral blood natural killer cells for adoptive cell therapy of B-cell precursor acute lymphoblastic leukemia

  • C. Quintarelli
  • , S. Sivori
  • , S. Caruso
  • , S. Carlomagno
  • , M. Falco
  • , I. Boffa
  • , D. Orlando
  • , M. Guercio
  • , Z. Abbaszadeh
  • , M. Sinibaldi
  • , S. Di Cecca
  • , A. Camera
  • , B. Cembrola
  • , A. Pitisci
  • , M. Andreani
  • , L. Vinti
  • , S. Gattari
  • , F. Del Bufalo
  • , M. Algeri
  • , G. Li Pira
  • A. Moseley, B. De Angelis, L. Moretta, Franco Locatelli

Risultato della ricerca: Contributo in rivistaArticolo

Abstract

We developed an innovative and efficient, feeder-free culture method to genetically modify and expand peripheral blood-derived NK cells with high proliferative capacity, while preserving the responsiveness of their native activating receptors. Activated peripheral blood NK cells were efficiently transduced by a retroviral vector, carrying a second-generation CAR targeting CD19. CAR expression was demonstrated across the different NK-cell subsets. CAR.CD19-NK cells display higher antileukemic activity toward CD19+ cell lines and primary blasts obtained from patients with B-cell precursor ALL compared with unmodified NK cells. In vivo animal model data showed that the antileukemia activity of CAR.CD19-NK cell is superimposable to that of CAR-T cells, with a lower xenograft toxicity profile. These data support the feasibility of generating feeder-free expanded, genetically modified peripheral blood NK cells for effective “off-the-shelf” immuno-gene-therapy, while their innate alloreactivity can be safely harnessed to potentiate allogeneic cell therapy.
Lingua originaleInglese
pagine (da-a)1102-1115
Numero di pagine14
RivistaLeukemia
Volume34
DOI
Stato di pubblicazionePubblicato - 2020

Keywords

  • NK
  • car

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