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Large Scale Ex Vivo Expansion of γδ T cells Using Artificial Antigen-presenting Cells.


ABSTRACT: Higher γδ T cell counts in patients with malignancies are associated with better survival. However, γδ T cells are rare in the blood and functionally impaired in patients with malignancies. Promising results are reported on the treatment of various malignancies with in vivo expansion of autologous γδ T cells using zoledronic acid (zol) and interleukin-2 (IL-2). Here we demonstrated that zol and IL-2, in combination with a novel genetically engineered K-562 CD3scFv/CD137L/CD28scFv/IL15RA quadruplet artificial antigen-presenting cell (aAPC), efficiently expand allogeneic donor-derived γδ T cells using a Good Manufacturing Practice (GMP) compliant protocol sufficient to achieve cell doses for future clinical use. We achieved a 633-fold expansion of γδ T cells after day 10 of coculture with aAPC, which exhibited central (47%) and effector (43%) memory phenotypes. In addition, >90% of the expanded γδ T cells expressed NKG2D, although they have low cell surface expression of PD1 and LAG3 inhibitory checkpoint receptors. In vitro real-time cytotoxicity analysis showed that expanded γδ T cells were effective in killing target cells. Our results demonstrate that large-scale ex vivo expansion of donor-derived γδ T cells in a GMP-like setting can be achieved with the use of quadruplet aAPC and zol/IL-2 for clinical application.

SUBMITTER: Boucher JC 

PROVIDER: S-EPMC9722378 | biostudies-literature | 2023 Jan

REPOSITORIES: biostudies-literature

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Large Scale Ex Vivo Expansion of γδ T cells Using Artificial Antigen-presenting Cells.

Boucher Justin C JC   Yu Bin B   Li Gongbo G   Shrestha Bishwas B   Sallman David D   Landin Ana Marie AM   Cox Cheryl C   Karyampudi Kumar K   Anasetti Claudio C   Davila Marco L ML   Bejanyan Nelli N  

Journal of immunotherapy (Hagerstown, Md. : 1997) 20221116 1


Higher γδ T cell counts in patients with malignancies are associated with better survival. However, γδ T cells are rare in the blood and functionally impaired in patients with malignancies. Promising results are reported on the treatment of various malignancies with in vivo expansion of autologous γδ T cells using zoledronic acid (zol) and interleukin-2 (IL-2). Here we demonstrated that zol and IL-2, in combination with a novel genetically engineered K-562 CD3scFv/CD137L/CD28scFv/IL15RA quadrupl  ...[more]

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