T-cell receptor gene transfer exclusively to human CD8(+) cells enhances tumor cell killing.

نویسندگان

  • Qi Zhou
  • Irene C Schneider
  • Inan Edes
  • Annemarie Honegger
  • Patricia Bach
  • Kurt Schönfeld
  • Axel Schambach
  • Winfried S Wels
  • Sabrina Kneissl
  • Wolfgang Uckert
  • Christian J Buchholz
چکیده

Transfer of tumor-specific T-cell receptor (TCR) genes into patient T cells is a promising strategy in cancer immunotherapy. We describe here a novel vector (CD8-LV) derived from lentivirus, which delivers genes exclusively and specifically to CD8(+) cells. CD8-LV mediated stable in vitro and in vivo reporter gene transfer as well as efficient transfer of genes encoding TCRs recognizing the melanoma antigen tyrosinase. Strikingly, T cells genetically modified with CD8-LV killed melanoma cells reproducibly more efficiently than CD8(+) cells transduced with a conventional lentiviral vector. Neither TCR expression levels, nor the rate of activation-induced death of transduced cells differed between both vector types. Instead, CD8-LV transduced cells showed increased granzyme B and perforin levels as well as an up-regulation of CD8 surface expression in a small subpopulation of cells. Thus, a possible mechanism for CD8-LV enhanced tumor cell killing may be based on activation of the effector functions of CD8(+) T cells by the vector particle displaying OKT8-derived CD8-scFv and an increase of the surface density of CD8, which functions as coreceptor for tumor-cell recognition. CD8-LV represents a powerful novel vector for TCR gene therapy and other applications in immunotherapy and basic research requiring CD8(+) cell-specific gene delivery.

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عنوان ژورنال:
  • Blood

دوره 120 22  شماره 

صفحات  -

تاریخ انتشار 2012