Literature DB >> 33148626

iPSC-derived NK cells maintain high cytotoxicity and enhance in vivo tumor control in concert with T cells and anti-PD-1 therapy.

Frank Cichocki1, Ryan Bjordahl2, Svetlana Gaidarova2, Sajid Mahmood2, Ramzey Abujarour2, Hongbo Wang1, Katie Tuininga1, Martin Felices1, Zachary B Davis1, Laura Bendzick1, Raedun Clarke2, Laurel Stokely2, Paul Rogers2, Moyar Ge2, Megan Robinson2, Betsy Rezner2, David L Robbins2, Tom T Lee2, Dan S Kaufman3, Bruce R Blazar4, Bahram Valamehr5, Jeffrey S Miller6.   

Abstract

The development of immunotherapeutic monoclonal antibodies targeting checkpoint inhibitory receptors, such as programmed cell death 1 (PD-1), or their ligands, such as PD-L1, has transformed the oncology landscape. However, durable tumor regression is limited to a minority of patients. Therefore, combining immunotherapies with those targeting checkpoint inhibitory receptors is a promising strategy to bolster antitumor responses and improve response rates. Natural killer (NK) cells have the potential to augment checkpoint inhibition therapies, such as PD-L1/PD-1 blockade, because NK cells mediate both direct tumor lysis and T cell activation and recruitment. However, sourcing donor-derived NK cells for adoptive cell therapy has been limited by both cell number and quality. Thus, we developed a robust and efficient manufacturing system for the differentiation and expansion of high-quality NK cells derived from induced pluripotent stem cells (iPSCs). iPSC-derived NK (iNK) cells produced inflammatory cytokines and exerted strong cytotoxicity against an array of hematologic and solid tumors. Furthermore, we showed that iNK cells recruit T cells and cooperate with T cells and anti-PD-1 antibody, further enhancing inflammatory cytokine production and tumor lysis. Because the iNK cell derivation process uses a renewable starting material and enables the manufacturing of large numbers of doses from a single manufacture, iNK cells represent an "off-the-shelf" source of cells for immunotherapy with the capacity to target tumors and engage the adaptive arm of the immune system to make a "cold" tumor "hot" by promoting the influx of activated T cells to augment checkpoint inhibitor therapies.
Copyright © 2020 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.

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Year:  2020        PMID: 33148626      PMCID: PMC8861807          DOI: 10.1126/scitranslmed.aaz5618

Source DB:  PubMed          Journal:  Sci Transl Med        ISSN: 1946-6234            Impact factor:   17.956


  61 in total

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Review 2.  T cell exhaustion.

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Journal:  Sci Transl Med       Date:  2016-09-21       Impact factor: 17.956

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Authors:  R Manetti; P Parronchi; M G Giudizi; M P Piccinni; E Maggi; G Trinchieri; S Romagnani
Journal:  J Exp Med       Date:  1993-04-01       Impact factor: 14.307

10.  Checkpoint blockade cancer immunotherapy targets tumour-specific mutant antigens.

Authors:  Matthew M Gubin; Xiuli Zhang; Heiko Schuster; Etienne Caron; Jeffrey P Ward; Takuro Noguchi; Yulia Ivanova; Jasreet Hundal; Cora D Arthur; Willem-Jan Krebber; Gwenn E Mulder; Mireille Toebes; Matthew D Vesely; Samuel S K Lam; Alan J Korman; James P Allison; Gordon J Freeman; Arlene H Sharpe; Erika L Pearce; Ton N Schumacher; Ruedi Aebersold; Hans-Georg Rammensee; Cornelis J M Melief; Elaine R Mardis; William E Gillanders; Maxim N Artyomov; Robert D Schreiber
Journal:  Nature       Date:  2014-11-27       Impact factor: 49.962

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  48 in total

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4.  Enhanced development of functional human NK cells in NOD-scid-IL2rgnull mice expressing human IL15.

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Review 5.  Implications for Immunotherapy of Breast Cancer by Understanding the Microenvironment of a Solid Tumor.

Authors:  Alexander S Franzén; Martin J Raftery; Gabriele Pecher
Journal:  Cancers (Basel)       Date:  2022-06-29       Impact factor: 6.575

Review 6.  Natural Killer Cells and Regulatory T Cells Cross Talk in Hepatocellular Carcinoma: Exploring Therapeutic Options for the Next Decade.

Authors:  Amber G Bozward; Frazer Warricker; Ye H Oo; Salim I Khakoo
Journal:  Front Immunol       Date:  2021-04-30       Impact factor: 7.561

Review 7.  Harnessing organs-on-a-chip to model tissue regeneration.

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Journal:  Cell Stem Cell       Date:  2021-06-03       Impact factor: 25.269

8.  Harnessing features of adaptive NK cells to generate iPSC-derived NK cells for enhanced immunotherapy.

Authors:  Karrune V Woan; Hansol Kim; Ryan Bjordahl; Zachary B Davis; Svetlana Gaidarova; John Goulding; Brian Hancock; Sajid Mahmood; Ramzey Abujarour; Hongbo Wang; Katie Tuininga; Bin Zhang; Cheng-Ying Wu; Behiye Kodal; Melissa Khaw; Laura Bendzick; Paul Rogers; Moyar Qing Ge; Greg Bonello; Miguel Meza; Martin Felices; Janel Huffman; Thomas Dailey; Tom T Lee; Bruce Walcheck; Karl J Malmberg; Bruce R Blazar; Yenan T Bryceson; Bahram Valamehr; Jeffrey S Miller; Frank Cichocki
Journal:  Cell Stem Cell       Date:  2021-09-14       Impact factor: 25.269

Review 9.  Bi-specific and Tri-specific NK Cell Engagers: The New Avenue of Targeted NK Cell Immunotherapy.

Authors:  Shee Kwan Phung; Jeffrey S Miller; Martin Felices
Journal:  Mol Diagn Ther       Date:  2021-07-29       Impact factor: 4.074

10.  Anti-NKG2C/IL-15/anti-CD33 killer engager directs primary and iPSC-derived NKG2C+ NK cells to target myeloid leukemia.

Authors:  Emily Chiu; Martin Felices; Frank Cichocki; Zachary Davis; Hongbo Wang; Katie Tuninga; Daniel A Vallera; Tom Lee; Ryan Bjordahl; Karl Johan Malmberg; Bahram Valamehr; Jeffrey S Miller
Journal:  Mol Ther       Date:  2021-06-24       Impact factor: 11.454

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