Application of dual affinity retargeting molecules to achieve optimal redirected T-cell killing of B-cell lymphoma.

نویسندگان

  • Paul A Moore
  • Wenjun Zhang
  • G Jonah Rainey
  • Steve Burke
  • Hua Li
  • Ling Huang
  • Sergey Gorlatov
  • Maria Concetta Veri
  • Sudeepta Aggarwal
  • Yinhua Yang
  • Kalpana Shah
  • Linda Jin
  • Sunan Zhang
  • Leilei He
  • Tengfei Zhang
  • Valentina Ciccarone
  • Scott Koenig
  • Ezio Bonvini
  • Syd Johnson
چکیده

We describe the application of a novel, bispecific antibody platform termed dual affinity retargeting (DART) to eradicate B-cell lymphoma through coengagement of the B cell-specific antigen CD19 and the TCR/CD3 complex on effector T cells. Comparison with a single-chain, bispecific antibody bearing identical CD19 and CD3 antibody Fv sequences revealed DART molecules to be more potent in directing B-cell lysis. The enhanced activity with the CD19xCD3 DART molecules was observed on all CD19-expressing target B cells evaluated using resting and prestimulated human PBMCs or purified effector T-cell populations. Characterization of a CD19xTCR bispecific DART molecule revealed equivalent potency with the CD19xCD3 DART molecule, demonstrating flexibility of the DART structure to support T-cell/B-cell associations for redirected T cell-killing applications. The enhanced level of killing mediated by DART molecules was not accompanied by any increase in nonspecific T-cell activation or lysis of CD19(-) cells. Cell-association studies indicated that the DART architecture is well suited for maintaining cell-to-cell contact, apparently contributing to the high level of target cell killing. Finally, the ability of the CD19xTCR DART to inhibit B-cell lymphoma in NOD/SCID mice when coadministered with human PBMCs supports further evaluation of DART molecules for the treatment of B-cell malignancies.

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عنوان ژورنال:
  • Blood

دوره 117 17  شماره 

صفحات  -

تاریخ انتشار 2011