Stimulation of natural killer cells with rhCD137 ligand enhances tumor-targeting antibody efficacy in gastric cancer

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RESEARCH PRODUCT

Stimulation of natural killer cells with rhCD137 ligand enhances tumor-targeting antibody efficacy in gastric cancer

Hideki Ohdan Nobuaki Fujikuni Toshihiro Misumi Kazuaki Tanabe

subject

0301 basic medicine Physiology Cytotoxicity Cancer Treatment lcsh:Medicine NK cells Toxicology Pathology and Laboratory Medicine Antineoplastic Agents Immunological Spectrum Analysis Techniques 0302 clinical medicine Immune Physiology Cellular types lcsh:Science Innate Immune System Cytotoxicity Assay Multidisciplinary biology Chemistry Immune cells CD137 Drug Synergism Flow Cytometry Recombinant Proteins Up-Regulation Gene Expression Regulation Neoplastic Killer Cells Natural Oncology Spectrophotometry 030220 oncology & carcinogenesis Cytokines White blood cells Female Tumor necrosis factor alpha Cytophotometry Antibody Research Article Cell biology Blood cells Cell Survival medicine.drug_class Immunology Antibodies Monoclonal Humanized Research and Analysis Methods Monoclonal antibody 03 medical and health sciences Immune system Stomach Neoplasms Cell Line Tumor Gastrointestinal Tumors medicine Humans Secretion Cell Proliferation Medicine and health sciences Biology and life sciences lcsh:R Cancers and Neoplasms Cancer Trastuzumab Molecular Development medicine.disease Granzyme B Gastric Cancer 4-1BB Ligand 030104 developmental biology Animal cells Immune System Cancer cell Cancer research biology.protein lcsh:Q Physiological Processes Developmental Biology

description

Although many anticancer agents for gastric cancer have been developed, the prognosis for many patients remains poor. Recently, costimulatory immune molecules that reactivate antitumor immune responses by utilizing the host immune system have attracted attention as new therapeutic strategies. CD137 is a costimulatory molecule that reportedly potentiates the antitumor activity of tumor-targeting monoclonal antibodies (mAbs) by enhancing antibody-dependent cellular cytotoxicity. However, it remains unclear whether CD137 stimulates tumor-regulatory activity in gastric cancer. In this study, we investigated the antitumor effects of CD137 stimulation on gastric cancer cells administered tumor-targeting mAbs. Our results showed that human natural killer (NK) cells were activated by expressing CD137 after encountering trastuzumab-coated gastric cancer cells, and that stimulation of activated NK cells in the presence of trastuzumab and recombinant human CD137 ligand (rhCD137L) enhanced cytotoxicity and release of cytokines (IFN-γ, TNF, granzyme A, or granzyme B) as compared with activated NK cells with trastuzumab alone (p < 0.05). By combination treatment with rhCD137L, similar effects were obtained regarding cancer cell cytotoxicity in the presence of cetuximab (p < 0.01). Moreover, we revealed that CD137 expression was dependent upon the affinity between the Fc portion of the antibodies and FcγRIIIa of NK cells based on results indicating that human IgG1 and IgG3 subclasses enhanced CD137 expression (p < 0.001). These results confirmed that FcγRIIIA polymorphisms (158 V/V) enhanced CD137 expression to a greater degree than 158 F polymorphisms (p = 0.014). Our results suggested that CD137 stimulation could promote the effects of tumor-targeting mAbs in gastric cancer, and that further investigation of antibody binding affinity and in vivo activities might improve therapeutic strategies related to the treatment of gastric cancer patients.

year	journal	country	edition	language
2018-08-21	PLOS ONE

https://doi.org/10.1371/journal.pone.0204880