Highly activated and expanded natural killer cells for multiple myeloma immunotherapy.

نویسندگان

  • Tarun K Garg
  • Susann M Szmania
  • Junaid A Khan
  • Antje Hoering
  • Paul A Malbrough
  • Amberly Moreno-Bost
  • Amy D Greenway
  • Joshuah D Lingo
  • Xin Li
  • Shmuel Yaccoby
  • Larry J Suva
  • Brian Storrie
  • Guido Tricot
  • Dario Campana
  • John D Shaughnessy
  • Bijay P Nair
  • William T Bellamy
  • Joshua Epstein
  • Bart Barlogie
  • Frits van Rhee
چکیده

BACKGROUND Patients with gene expression profiling-defined high-risk myeloma in relapse have poor outcomes with current therapies. We tested whether natural killer cells expanded by co-culture with K562 cells transfected with 41BBL and membrane-bound interleukin-15 could kill myeloma cells with a high-risk gene expression profile in vitro and in a unique model which recapitulates human myeloma. DESIGN AND METHODS OPM2 and high-risk primary myeloma tumors were grown in human fetal bone implanted into non-obese diabetic severe combined immunodeficiency mice with a deficient interleukin-2 receptor gamma chain. These mice are devoid of endogenous natural killer and T-cell activity and were used to determine whether adoptively transferred expanded natural killer cells could inhibit myeloma growth and myeloma-associated bone destruction. RESULTS Natural killer cells from healthy donors and myeloma patients expanded a median of 804- and 351-fold, respectively, without significant T-cell expansion. Expanded natural killer cells killed both allogeneic and autologous primary myeloma cells avidly via a perforin-mediated mechanism in which the activating receptor NKG2D, natural cytotoxicity receptors, and DNAX-accessory molecule-1 played a central role. Adoptive transfer of expanded natural killer cells inhibited the growth of established OPM2 and high-risk primary myeloma tumors grown in the murine model. The transferred, expanded natural killer cells proliferated in vivo in an interleukin-2 dose-dependent fashion, persisted up to 4 weeks, were readily detectable in the human bone, inhibited myeloma growth and protected bone from myeloma-induced osteolysis. CONCLUSIONS These studies provide the rationale for testing expanded natural killer cells in humans.

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عنوان ژورنال:
  • Haematologica

دوره 97 9  شماره 

صفحات  -

تاریخ انتشار 2012