Sequential Exposure to IL21 and IL15 During Human Natural Killer Cell Expansion Optimizes Yield and Function

Author:

Zhang Caimei1ORCID,Kadu Siddhant1ORCID,Xiao Yansen1ORCID,Johnson Omar1ORCID,Kelly Andre12ORCID,O'Connor Roddy S.12ORCID,Lai Meizan1ORCID,Kong Hong1ORCID,Srivatsa Sriram1ORCID,Tai Victoria1ORCID,Greenblatt Eli3ORCID,Holmes Matthew3ORCID,Riley James L.14ORCID,June Carl H.12ORCID,Sheppard Neil C.12ORCID

Affiliation:

1. 1Center for Cellular Immunotherapies, University of Pennsylvania, Philadelphia, Pennsylvania.

2. 2Department of Pathology and Laboratory Medicine, Perelman School of Medicine, University of Pennsylvania, Philadelphia.

3. 3IsoPlexis, Branford, Connecticut.

4. 4Department of Microbiology, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania.

Abstract

Abstract Natural killer (NK) cells are frequently expanded for the clinic using irradiated, engineered K562 feeder cells expressing a core transgene set of membrane-bound (mb) IL15 and/or mbIL21 together with 41BBL. Prior comparisons of mbIL15 to mbIL21 for NK expansion lack comparisons of key attributes of the resulting NK cells, including their high-dimensional phenotype, polyfunctionality, the breadth and potency of cytotoxicity, cellular metabolism, and activity in xenograft tumor models. Moreover, despite multiple rounds of K562 stimulation, studies of sequential use of mbIL15- and mbIL21-based feeder cells are absent. We addressed these gaps and found that using mbIL15- versus mbIL21-based feeder cells drove distinct phenotypic and functional profiles. Feeder cells expressing mbIL15 alone drove superior functionality by nearly all measures, whereas those expressing mbIL21 alone drove superior yield. In combination, most attributes resembled those imparted by mbIL21, whereas in sequence, NK yield approximated that imparted by the first cytokine, and the phenotype, transcriptome, and function resembled that driven by the second cytokine, highlighting the plasticity of NK cell differentiation. The sequence mbIL21 followed by mbIL15 was advantageous in achieving significant yields of highly functional NK cells that demonstrated equivalent in vivo activity to those expanded by mbIL15 alone in two of three xenograft models. Our findings define the impact of mbIL15 versus mbIL21 during NK expansion and reveal a previously underappreciated tradeoff between NK yield and function for which sequential use of mbIL21-based followed by mbIL15-based feeder cells may be the optimal approach in many settings.

Funder

University of Pennsylvania

National Cancer Institute

Ludwig Institute for Cancer Research

IsoPlexis

Publisher

American Association for Cancer Research (AACR)

Subject

Cancer Research,Immunology

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