Dmm021147 1401..1412

نویسندگان

  • Ceri E. Oldreive
  • Anna Skowronska
  • Nicholas J. Davies
  • Helen Parry
  • Angelo Agathanggelou
  • Sergey Krysov
  • Graham Packham
  • Zbigniew Rudzki
  • Laura Cronin
  • Katerina Vrzalikova
  • Paul Murray
  • Elena Odintsova
  • Guy Pratt
  • A. Malcolm R. Taylor
  • Paul Moss
  • Tatjana Stankovic
چکیده

Chronic lymphocytic leukaemia (CLL) cells require microenvironmental support for their proliferation. This can be recapitulated in highly immunocompromised hosts in the presence of T cells and other supporting cells. Current primary CLL xenograft models suffer from limited duration of tumour cell engraftment coupled with gradual T-cell outgrowth. Thus, a greater understanding of the interaction between CLL and T cells could improve their utility. In this study, using two distinct mouse xenograft models, we investigated whether xenografts recapitulate CLL biology, including natural environmental interactions with B-cell receptors and T cells, andwhethermanipulation of autologous T cells can expand the duration of CLL engraftment. We observed that primary CLL xenografts recapitulated both the tumour phenotype and T-cell repertoire observed in patients and that engraftment was significantly shorter for progressive tumours. A reduction in the number of patient T cells that were injected into the mice to 2-5% of the initial number or specific depletion of CD8 cells extended the limited xenograft duration of progressive cases to that characteristic of indolent disease. We conclude that manipulation of T cells can enhance current CLL xenograft models and thus expand their utility for investigation of tumour biology and pre-clinical drug

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تاریخ انتشار 2015