Syngeneic natural killer cell therapy activates dendritic and T cells in metastatic lungs and effectively treat low-burden metastases

Author:

Huang Shih-Wen12,Lai Yein-Gei1,Liao Hao-Ting13ORCID,Chang Chin-Ling1,Ma Ruo-Yu1,Chen Yung-Hsiang1,Liou Yae-Huei1,Wu Zhen-Qi1,Wu Yu-Chen4,Liu Ko-Jiunn4,Huang Yen-Tsung5,Yang Jen-Lung1,Dai Ming-Shen6,Liao Nan-Shih12ORCID

Affiliation:

1. Institute of Molecular Biology, Academia Sinica

2. Molecular and Cell Biology, Taiwan International Graduate Program, Academia Sinica and Graduate Institute of Life Science, National Defense Medical Center

3. Department of Life Sciences, National Central University

4. National Institute of Cancer Research, National Health Research Institutes

5. Institute of Statistical Science, Academia Sinica

6. Department of Hematology-Oncology, Tri-Service General Hospital

Abstract

Natural killer (NK) cells can control metastasis through cytotoxicity and IFN-γ production independently of T cells in experimental metastasis mouse models. The inverse correlation between NK activity and metastasis incidence supports a critical role for NK cells in human metastatic surveillance. However, autologous NK cell therapy has shown limited benefit in treating patients with metastatic solid tumors. Using a spontaneous metastasis mouse model of MHC-I + breast cancer, we found that transfer of IL-15/IL-12-conditioned syngeneic NK cells after primary tumor resection promoted long-term survival of mice with low metastatic burden and induced a tumor-specific protective T cell response that is essential for the therapeutic effect. Furthermore, NK cell transfer augments activation of conventional dendritic cells (cDCs), Foxp3 - CD4 + T cells and stem cell-like CD8 + T cells in metastatic lungs, which requires IFN-γ of the transferred NK cells. These results imply direct interactions between transferred NK cells and endogenous cDCs to enhance T cell activation. We conducted an investigator-initiated clinical trial of autologous NK cell therapy in six patients with advanced cancer and observed that the NK cell therapy was safe and showed signs of effectiveness. These findings indicate that autologous NK cell therapy is effective in treating established low burden metastases of MHC-I + tumor cells by activating the cDC-T cell axis at metastatic sites.

Publisher

eLife Sciences Publications, Ltd

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