Clinical implications of monitoring nivolumab immunokinetics in non–small cell lung cancer patients
Akio Osa, … , Takashi Kijima, Atsushi Kumanogoh
Akio Osa, … , Takashi Kijima, Atsushi Kumanogoh
Published October 4, 2018
Citation Information: JCI Insight. 2018;3(19):e59125. https://doi.org/10.1172/jci.insight.59125.
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Clinical Medicine Immunology Pulmonology

Clinical implications of monitoring nivolumab immunokinetics in non–small cell lung cancer patients

Abstract

BACKGROUND. The PD-1–blocking antibody nivolumab persists in patients several weeks after the last infusion. However, no study has systematically evaluated the maximum duration that the antibody persists on T cells or the association between this duration and residual therapeutic efficacy or potential adverse events. METHODS. To define the duration of binding and residual efficacy of nivolumab after discontinuation, we developed a simplified strategy for T cell monitoring and used it to analyze T cells from peripheral blood from 11 non–small cell lung cancer patients previously treated with nivolumab. To determine the suitability of our method for other applications, we compared transcriptome profiles between nivolumab-bound and nivolumab-unbound CD8 T cells. We also applied T cell monitoring in 2 nivolumab-treated patients who developed progressive lung tumors during long-term follow-up. RESULTS. Prolonged nivolumab binding was detected more than 20 weeks after the last infusion, regardless of the total number of nivolumab infusions (2–15 doses) or type of subsequent treatment, in 9 of the 11 cases in which long-term monitoring was possible. Ki-67 positivity, a proliferation marker, in T cells decreased in patients with progressive disease. Transcriptome profiling identified the signals regulating activation of nivolumab-bound T cells, which may contribute to nivolumab resistance. In 2 patients who restarted nivolumab, T cell proliferation markers exhibited the opposite trend and correlated with clinical response. CONCLUSIONS. Although only a few samples were analyzed, our strategy of monitoring both nivolumab binding and Ki-67 in T cells might help determine residual efficacy under various types of concurrent or subsequent treatment. TRIAL REGISTRATION. University Hospital Medical Information Network Clinical Trials Registry, UMIN000024623. FUNDING. This work was supported by Japan Society for the Promotion of Science KAKENHI (JP17K16045, JP18H05282, and JP15K09220), Japan Agency for Medical Research and Development (JP17cm0106310, JP18cm0106335 and JP18cm059042), and Core Research for Evolutional Science and Technology (JPMJCR16G2).

Authors

Akio Osa, Takeshi Uenami, Shohei Koyama, Kosuke Fujimoto, Daisuke Okuzaki, Takayuki Takimoto, Haruhiko Hirata, Yukihiro Yano, Soichiro Yokota, Yuhei Kinehara, Yujiro Naito, Tomoyuki Otsuka, Masaki Kanazu, Muneyoshi Kuroyama, Masanari Hamaguchi, Taro Koba, Yu Futami, Mikako Ishijima, Yasuhiko Suga, Yuki Akazawa, Hirotomo Machiyama, Kota Iwahori, Hyota Takamatsu, Izumi Nagatomo, Yoshito Takeda, Hiroshi Kida, Esra A. Akbay, Peter S. Hammerman, Kwok-kin Wong, Glenn Dranoff, Masahide Mori, Takashi Kijima, Atsushi Kumanogoh

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Figure 3

The change in nivolumab-binding status can be mapped by flow cytometry.

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The change in nivolumab-binding status can be mapped by flow cytometry. ...
(A) Human PD-1–transfected HEK293T cells (HEK293T-PD-1) were treated with serial dilutions of nivolumab (10, 2, 0.4, 0.08, 0.016, and 0.0032 μg/ml), and the staining patterns of IgG4 and PD-1 detection antibodies and the capacity of recombinant PD-L1 binding (20 μg/ml) were evaluated. Data are representative of 3 independent experiments. (B) Schematics present 3 different binding statuses: complete binding (CB: red gate), partial binding (PB: blue gate), and no binding (NB: green gate). (C) Nivolumab binding was analyzed at 2 follow-up time points, as indicated, in fresh peripheral blood CD8 and CD4 T cells from each of 3 cases that discontinued treatment (Pt. 5–7).