A novel combination therapy of arginine deiminase and an arginase inhibitor targeting arginine metabolism in the tumor and immune microenvironment

Pei-Hsuan Ye; Chung-Yen Li; Hao-Yu Cheng; Gangga Anuraga; Chih-Yang Wang; Feng-Wei Chen; Shiang-Jie Yang; Kuo-Ting Lee; Kwang-Yu Chang; Ming-Derg Lai

A novel combination therapy of arginine deiminase and an arginase inhibitor targeting arginine metabolism in the tumor and immune microenvironment

Am J Cancer Res. 2023 May 15;13(5):1952-1969. eCollection 2023.

Authors

Pei-Hsuan Ye¹, Chung-Yen Li², Hao-Yu Cheng³, Gangga Anuraga^{4

5}, Chih-Yang Wang⁴, Feng-Wei Chen², Shiang-Jie Yang², Kuo-Ting Lee⁶, Kwang-Yu Chang^{7

8}, Ming-Derg Lai^{1

2}

Affiliations

¹ Department of Biochemistry and Molecular Biology, College of Medicine, National Cheng Kung University Tainan, Taiwan, ROC.
² Institute of Basic Medical Sciences, College of Medicine, National Cheng Kung University Tainan, Taiwan, ROC.
³ Department of Biotechnology and Bioindustry Sciences, National Cheng Kung University Tainan, Taiwan, ROC.
⁴ PhD Program for Cancer Molecular Biology and Drug Discovery, College of Medical Science and Technology, Taipei Medical University and Academia Sinica Taipei, Taiwan, ROC.
⁵ Department of Biological Science, Faculty of Science and Technology, Universitas PGRI Adi Buana Surabaya 60234, Indonesia.
⁶ Department of Surgery, National Cheng Kung University Hospital, College of Medicine, National Cheng Kung University Tainan, Taiwan, ROC.
⁷ National Institute of Cancer Research, National Health Research Institutes Tainan, Taiwan, ROC.
⁸ Department of Oncology, National Cheng Kung University Hospital, College of Medicine, National Cheng Kung University Tainan, Taiwan, ROC.

PMID: 37293150
PMCID: PMC10244097

Abstract

Tumor progression is dependent on tumor cells and their microenvironment. It is important to identify therapies that inhibit cancer cells and activate immune cells. Arginine modulation plays a dual role in cancer therapy. Arginase inhibition induced an anti-tumor effect via T-cell activation through an increase in arginine in the tumor environment. In contrast, arginine depletion by arginine deiminase pegylated with 20,000-molecular-weight polyethylene glycol (ADI-PEG 20) induced an anti-tumor response in argininosuccinate synthase 1 (ASS1)-deficient tumor cells. ADI-PEG 20 did not cause toxicity to normal immune cells, which can recycle the ADI-degraded product citrulline back to arginine. To target tumor cells and their neighboring immune cells, we hypothesized that the combination of an arginase inhibitor (L-Norvaline) and ADI-PEG 20 may trigger a stronger anticancer response. In this study, we found that L-Norvaline inhibits tumor growth in vivo. Pathway analysis based on RNA-seq data indicated that the differentially expressed genes (DEGs) were significantly enriched in some immune-related pathways. Significantly, L-Norvaline did not inhibit tumor growth in immunodeficient mice. In addition, combination treatment with L-Norvaline and ADI-PEG 20 induced a more robust anti-tumor response against B16F10 melanoma. Furthermore, single-cell RNA-seq data demonstrated that the combination therapy increased tumor-infiltrating CD8⁺ T cells and CCR7⁺ dendritic cells. The increase in infiltrated dendritic cells may enhance the anti-tumor response of CD8⁺ cytotoxic T cells, indicating a potential mechanism for the observed anti-tumor effect of the combination treatment. In addition, populations of immunosuppressive-like immune cells, such as S100a8⁺ S100a9⁺ monocytes and Retnla⁺ Retnlg⁺ TAMs, in tumors were dramatically decreased. Importantly, mechanistic analysis indicated that the processes of the cell cycle, ribonucleoprotein complex biogenesis, and ribosome biogenesis were upregulated after combination treatment. This study implied the possibility of L-Norvaline as a modulator of the immune response in cancer and provided a new potential therapy combined with ADI-PEG 20.

Keywords: ADI-PEG 20; arginase inhibitor; arginine metabolism; immune modulation; single-cell RNA sequencing; tumor microenvironment.