Chemical priming of natural killer cells with branched polyethylenimine for cancer immunotherapy

Seung Hee Choi; Hye Jin Kim; Joo Dong Park; Eun-Su Ko; Minwook Lee; Dae-Keum Lee; Jin-Ho Choi; Hye Jung Jang; Isaac Kim; Hae-Yun Jung; Keun-Hong Park; Kyung-Soon Park

doi:10.1136/jitc-2022-004964

Chemical priming of natural killer cells with branched polyethylenimine for cancer immunotherapy

J Immunother Cancer. 2022 Aug;10(8):e004964. doi: 10.1136/jitc-2022-004964.

Authors

Affiliations

¹ Department of Biomedical Science, CHA University, Seongnam-si, Korea (the Republic of).
² Department of Surgery, Bundang CHA Medical Center, CHA University, Seongnam-si, Korea (the Republic of).
³ Department of Biomedical Science, CHA University, Seongnam-si, Korea (the Republic of) pkh0410@cha.ac.kr kspark@cha.ac.kr.

^# Contributed equally.

Abstract

Background: Due to their powerful immune surveillance activity and ability to kill and clear cancer cells, natural killer (NK) cells are an emerging anticancer immunotherapeutic agent. Therefore, there is much interest in developing efficient technologies that further enhance the therapeutic antitumor efficacy of NK cells.

Methods: To produce chemically primed NK cells, we screened polymers with various electric charges and examined their ability to enhance the cytotoxicity of NK cells. The effect of primary amine and electric charges of 25 kDa branched polyethylenimine (25KbPEI) was investigated by fluorination of the chemical. The role of 25KbPEI in determining the major priming mechanism was investigated in terms of calcium influx into NK cells. In vivo therapeutic efficacy of chemically primed NK cells was evaluated against solid tumor mouse model of triple negative breast and ovarian cancers.

Results: Chem_NK that was produced by the priming activity of 25KbPEI showed potent antitumor activity to various cancer cells. Chem_NK showed an activated phenotype, which manifests as increased expression of activating/adhesion/chemokine receptors and perforin accumulation, leading to enhanced migration ability and antitumor activity. Chem_NK display potent therapeutic efficacy against in vivo mouse model of triple negative breast and ovarian cancers. Fluorination of the primary amine group reduces the activity of 25KbPEI to prime NK cells, indicating that the cationic charge on the chemical plays a critical role in NK cell activation. A major priming mechanism was 25KbPEI-mediated calcium influx into NK cells, which occurred mainly via the Ca2⁺-permeable non-selective cation channel transient receptor potential melastatin 2.

Conclusions: NK cells can be chemically primed with 25KbPEI to express potent antitumor activity as well as enhanced migration ability. Because PEI is a biocompatible and Food and Drug Administration-approved chemical for biomedical use, these results suggest a cost-effective and simple method of producing therapeutic NK cells.

Keywords: immunity, cellular; immunotherapy; killer cells, natural.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Amines
Animals
Antineoplastic Agents*
Calcium
Cell Line, Tumor
Female
Humans
Immunotherapy
Killer Cells, Natural
Mice
Ovarian Neoplasms*
Polyethyleneimine
Triple Negative Breast Neoplasms*
United States

Substances

Amines
Antineoplastic Agents
Polyethyleneimine
Calcium