Efficient ADCC killing of meningioma by avelumab and a high-affinity natural killer cell line, haNK
Amber J. Giles, Shuyu Hao, Michelle Padget, Hua Song, Wei Zhang, John Lynes, Victoria Sanchez, Yang Liu, Jinkyu Jung, Xiaoyu Cao, Rika Fujii, Randy Jensen, David Gillespie, Jeffrey Schlom, Mark R. Gilbert, Edjah K. Nduom, Chunzhang Yang, John H. Lee, Patrick Soon-Shiong, James W. Hodge, Deric M. Park
Amber J. Giles, Shuyu Hao, Michelle Padget, Hua Song, Wei Zhang, John Lynes, Victoria Sanchez, Yang Liu, Jinkyu Jung, Xiaoyu Cao, Rika Fujii, Randy Jensen, David Gillespie, Jeffrey Schlom, Mark R. Gilbert, Edjah K. Nduom, Chunzhang Yang, John H. Lee, Patrick Soon-Shiong, James W. Hodge, Deric M. Park
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Research Article Oncology Therapeutics

Efficient ADCC killing of meningioma by avelumab and a high-affinity natural killer cell line, haNK

Abstract

Meningiomas are the most common adult primary tumor of the central nervous system, but there are no known effective medical therapies for recurrent meningioma, particularly for World Health Organization grade II and III tumors. Meningiomas arise from the meninges, located outside the blood-brain barrier, and therefore may be directly targeted by antibody-mediated immunotherapy. We found that programmed cell death ligand 1 (PD-L1) was highly expressed in multiple human malignant meningioma cell lines and patient tumor samples. PD-L1 was targeted with the anti–PD-L1 antibody avelumab and directed natural killer cells to mediate antibody-dependent cellular cytotoxicity (ADCC) of PD-L1–expressing meningioma tumors both in vitro and in vivo. ADCC of meningioma cells was significantly increased in target cells that upregulated PD-L1 expression and, conversely, abrogated in tumor cells that were depleted of PD-L1. Additionally, the high-affinity natural killer cell line, haNK, outperformed healthy donor NK cells in meningioma ADCC. Together, these data support a clinical trial designed to target PD-L1 with avelumab and haNK cells, potentially offering a novel immunotherapeutic approach for patients with malignant meningioma.

Authors

Amber J. Giles, Shuyu Hao, Michelle Padget, Hua Song, Wei Zhang, John Lynes, Victoria Sanchez, Yang Liu, Jinkyu Jung, Xiaoyu Cao, Rika Fujii, Randy Jensen, David Gillespie, Jeffrey Schlom, Mark R. Gilbert, Edjah K. Nduom, Chunzhang Yang, John H. Lee, Patrick Soon-Shiong, James W. Hodge, Deric M. Park

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Figure 2

ADCC of meningioma is mediated by Fc receptor binding, and ADCC is increased with high-avidity Fc receptors.

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ADCC of meningioma is mediated by Fc receptor binding, and ADCC is incre...
(A) ADCC assay of malignant meningioma lines by healthy donor NK cells. Meningioma lines were incubated with avelumab alone, healthy donor NK cells and isotype antibody, or NK cells and avelumab. The ratio of NK to meningioma cells is indicated. Each sample was plated in triplicate. Data were analyzed with a 2-way ANOVA; *P < 0.05. Shown are representative data from 3 repeats using different healthy donors. (B) ADCC of IOMM incubated with avelumab or healthy donor NK cells with isotype, avelumab, or avelumab with α-CD16 (Fc-blocking) antibody. Data were analyzed with a 2-way ANOVA. (C) ADCC assay of 5 meningioma lines by NK cells from healthy donors with the F/F or V/V polymorphism of the CD16 receptor (effector/target [E/T] of 10:1). Data were analyzed with unpaired 1-tailed t test comparing NK and isotype with NK and avelumab conditions. (D) Lysis of IOMM meningioma by healthy donor NK cells versus haNK cells in the presence of avelumab. Samples were plated in triplicate. Data were analyzed with 1-way ANOVA.