Sufficiently activated mature natural killer cells derived from peripheral blood mononuclear cells substantially enhance antitumor activity

Chuanling Liu; Yingying Li; Yanrong Li; Meng Hu; Haiyan Wang; Shasha Lu; Zhao Li; Dilinuer Dilimulati; Shunchang Jiao; Shelian Lu; Weihong Zhao

doi:10.1002/iid3.1143

Immunity, Inflammation and Disease (Jan 2024)

Sufficiently activated mature natural killer cells derived from peripheral blood mononuclear cells substantially enhance antitumor activity

Chuanling Liu,
Yingying Li,
Yanrong Li,
Meng Hu,
Haiyan Wang,
Shasha Lu,
Zhao Li,
Dilinuer Dilimulati,
Shunchang Jiao,
Shelian Lu,
Weihong Zhao

Affiliations

Chuanling Liu: Department of Oncology Chinese PLA General Hospital Beijing China
Yingying Li: Research and Development Department Beijing DCTY® Biotech Co., Ltd Beijing China
Yanrong Li: Research and Development Department Beijing DCTY® Biotech Co., Ltd Beijing China
Meng Hu: Research and Development Department Beijing DCTY® Biotech Co., Ltd Beijing China
Haiyan Wang: Research and Development Department Beijing DCTY® Biotech Co., Ltd Beijing China
Shasha Lu: Research and Development Department Beijing DCTY® Biotech Co., Ltd Beijing China
Zhao Li: Research and Development Department Beijing DCTY® Biotech Co., Ltd Beijing China
Dilinuer Dilimulati: Research and Development Department Beijing DCTY® Biotech Co., Ltd Beijing China
Shunchang Jiao: Department of Oncology Chinese PLA General Hospital Beijing China
Shelian Lu: Research and Development Department Beijing DCTY® Biotech Co., Ltd Beijing China
Weihong Zhao: Department of Oncology Chinese PLA General Hospital Beijing China

DOI: https://doi.org/10.1002/iid3.1143
Journal volume & issue: Vol. 12, no. 1
pp. n/a – n/a

Abstract

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Abstract Background Peripheral blood‐derived natural killer (NK) cells spontaneously lyse tumor cells without prior sensitization. However, NK cells in peripheral blood (PBNK cells) are in a resting state and exhibit inhibitory phenotypes and impaired cytotoxicity. Thus, strengthening the cytotoxic effector function of PBNK cells and improving NK cell expansion in vitro for a convenient allogeneic therapy are essential. Materials and Methods Pure cytokine activation and expansion of NK cells (super NK [SNK]) from peripheral blood mononuclear cells were studied. Markers of activated and inhibited NK cells and cytokine secretion by NK cells were examined using flow cytometry. NK cell antitumor activity in vitro was assessed using lactate dehydrogenase (LDH) cytotoxicity assay and an Incucyte real‐time imaging system. Additionally, the function of SNK cells against ascites caused by ovarian cancer in NOD‐Prkdc(em26Cd52)il2rg(em26Cd22)/Nju (NCG) mice was determined. In a further investigation of the differences between PBNK and SNK, the mRNA of both cells was sequenced and analyzed. Results Human peripheral blood mononuclear cells showed selective NK cell expansion upon cytokine activation and culture. Both SNK and PBNK cells expressed activation markers, but at different levels, and SNK cells secreted more cytokines related to cytotoxicity than PBNK cells did. Accordingly, SNK cells exhibited strong antitumor activity ex vivo and improved NCG mice survival after intraperitoneal ovarian cancer transplantation. Mechanistically, SNK cells expressed more genes associated with nucleotide metabolism, fatty acid, and ATP metabolism than PBNK cells. Conclusion SNK cells derived from peripheral blood mononuclear cells have sufficiently activated mature characteristics and high antitumor activity, rendering them a highly promising and essential therapeutic approach for cancer treatment.

Published in Immunity, Inflammation and Disease

ISSN: 2050-4527 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: https://onlinelibrary.wiley.com/journal/20504527

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