Combination of cancer vaccine with CD122-biased IL-2/anti-IL-2 Ab complex shapes the stem-like effector NK and CD8+ T cells against tumor
Spotlight (1) Shimizu K (2) Ueda S (3) Kawamura M (4) Aoshima H (5) Satoh M (6) Nakabayashi J (7) Fujii SI
In combination with a WT1 vaccine in a model off advanced leukemia, Shimizu, Ueda, and Kawamura, et al. tested two IL-2/anti-IL-2 mAb complexes (IL-2Cxs) – S4B6, which is biased towards CD122 and expands NK cells and memory CD8+ T cells, and JES6, which is biased towards CD25 and expands Tregs. The combination with S4B6, but not JES6, induced 100% survival, dependent on T and NK cells. Treatment enhanced activation of NKT1 cells, expanded NK cells at immature and semi-mature stages, and increased distinct subsets of NK and CD8+ T cells with stem-like phenotypes. Memory CD8+ T cells capable of potent antitumor protection were maintained long-term.
Contributed by Lauren Hitchings
(1) Shimizu K (2) Ueda S (3) Kawamura M (4) Aoshima H (5) Satoh M (6) Nakabayashi J (7) Fujii SI
In combination with a WT1 vaccine in a model off advanced leukemia, Shimizu, Ueda, and Kawamura, et al. tested two IL-2/anti-IL-2 mAb complexes (IL-2Cxs) – S4B6, which is biased towards CD122 and expands NK cells and memory CD8+ T cells, and JES6, which is biased towards CD25 and expands Tregs. The combination with S4B6, but not JES6, induced 100% survival, dependent on T and NK cells. Treatment enhanced activation of NKT1 cells, expanded NK cells at immature and semi-mature stages, and increased distinct subsets of NK and CD8+ T cells with stem-like phenotypes. Memory CD8+ T cells capable of potent antitumor protection were maintained long-term.
Contributed by Lauren Hitchings
BACKGROUND: A key to success of cancer immunotherapy is the amplification and sustenance of various effector cells. The hallmark of prominent antitumor T cells is their long-term effector function. Although interleukin (IL)-2 is an attractive cytokine, several attempts have been made towards developing IL-2 modalities with improved effectiveness and safety that enhance natural killer (NK) cells or T cells in cancer models. However, whether such IL-2 modalities can simultaneously support long-term innate and adaptive immunity, particularly stem-like memory, has not been shown. To resolve this issue, we compared the antitumor cellular mechanism with two IL-2/anti-IL-2 complexes (IL-2Cxs) administered in combination with a therapeutic cancer vaccine, which we had previously established as an in vivo dendritic cell-targeting therapy. METHODS: Two types of IL-2Cxs, CD25-biased IL-2Cx and CD122-biased IL-2Cx, together with a Wilms' tumor 1-expressing vaccine, were evaluated in a leukemic model. The immunological response and synergistic antitumor efficacy of these IL-2Cxs were then evaluated. RESULTS: When CD25-biased or CD122-biased IL-2Cxs in combination with the vaccine were assessed in an advanced-leukemia model, the CD122-biased IL-2Cx combination showed 100% survival, but the CD25-biased IL-2Cx did not. We first showed that invariant natural killer T (NKT) 1 cells are predominantly activated by CD122-biased IL-2Cx. In addition, in-depth analysis of immune responses by CD122-biased IL-2Cx in lymphoid tissues and the tumor microenvironment revealed a dramatic increase in the distinct subsets of NK and CD8(+) T cells with stem-like phenotype (CD27(+)Sca-1(hi), CXCR3(hi), CD127(+)TCF-1(+)T-bet(+) Eomes(+)). Moreover, CD122-biased IL-2Cx combination therapy maintained long-term memory CD8(+) T cells capable of potent antitumor protection. After the high dimensional profiling analysis of NK and CD8(+)T cells, principal component analysis revealed that the stem-like-NK cell and stem-like-CD8(+)T cell state in the combination were integrated in the same group. CONCLUSIONS: CD122-biased IL-2Cx combined with the vaccine can induce a series of reactions in the immune cascade, including activation of not only NKT1 cells, but also NK and CD8(+) T cells with a stem-like memory phenotype. Since it can also lead to a long-term, strong antitumor response, the combination of CD122-biased IL-2Cx with a vaccine may serve as a potential and competent strategy for patients with advanced cancer.
Author Info: (1) Laboratory for Immunotherapy, RIKEN Center for Integrative Medical Sciences, Yokohama, Japan. Program for Drug Discovery and Medical Technology Platforms, RIKEN, Yokohama, Japa
Author Info: (1) Laboratory for Immunotherapy, RIKEN Center for Integrative Medical Sciences, Yokohama, Japan. Program for Drug Discovery and Medical Technology Platforms, RIKEN, Yokohama, Japan. (2) Laboratory for Immunotherapy, RIKEN Center for Integrative Medical Sciences, Yokohama, Japan. (3) Laboratory for Immunotherapy, RIKEN Center for Integrative Medical Sciences, Yokohama, Japan. (4) Laboratory for Immunotherapy, RIKEN Center for Integrative Medical Sciences, Yokohama, Japan. (5) Laboratory for Immunotherapy, RIKEN Center for Integrative Medical Sciences, Yokohama, Japan. (6) Department of Mathematics, Tokyo Medical and Dental University, Ichikawa, Japan. (7) Laboratory for Immunotherapy, RIKEN Center for Integrative Medical Sciences, Yokohama, Japan shin-ichiro.fujii@riken.jp. Program for Drug Discovery and Medical Technology Platforms, RIKEN, Yokohama, Japan.
Citation: J Immunother Cancer 2023 Jul 11: Epub
