Hepatocyte-derived FGL1 accelerates liver metastasis and tumor growth by inhibiting CD8+ T and NK cells
Fengjia Xi, … , Rui Sun, Yongyan Chen
Fengjia Xi, … , Rui Sun, Yongyan Chen
Published July 8, 2024
Citation Information: JCI Insight. 2024;9(13):e173215. https://doi.org/10.1172/jci.insight.173215.
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Research Article Hepatology Immunology

Hepatocyte-derived FGL1 accelerates liver metastasis and tumor growth by inhibiting CD8+ T and NK cells

Abstract

Fibrinogen-like protein 1 (FGL1) contributes to the proliferation and metabolism of hepatocytes; however, as a major ligand of the immune checkpoint, its role in the liver regional immune microenvironment is poorly understood. Hepatocytes specifically and highly expressed FGL1 under normal physiological conditions. Increases in hepatic CD8+ T and NK cell numbers and functions were found in Fgl1-deficient (Fgl1–/–) mice, but not in the spleen or lymph node, similar to findings in anti-FGL1 mAb–treated wild-type mice. Furthermore, Fgl1 deficiency or anti-FGL1 mAb blockade restrained liver metastasis and slowed the growth of orthotopic tumors, with significantly prolonged survival of tumor-bearing mice. Tumor-infiltrating hepatic CD8+ T and NK cells upregulated the expression of lymphocyte activation gene-3 (LAG-3) and exhibited stronger antitumor activities after anti-FGL1 treatment. The antitumor efficacy of FGL1 blockade depended on cytotoxic T lymphocytes and NK cells, demonstrated by using a cell-deficient mouse model and cell transfer in vivo. In vitro, FGL1 directly inhibited hepatic T and NK cells related to the receptor LAG-3. In conclusion, hepatocyte-derived FGL1 played critical immunoregulatory roles in the liver and contributed to liver metastasis and tumor growth by inhibiting CD8+ T and NK cell functions via the receptor LAG-3, providing a new strategy for liver cancer immunotherapy.

Authors

Fengjia Xi, Haoyu Sun, Hui Peng, Zhexiong Lian, Haiming Wei, Zhigang Tian, Rui Sun, Yongyan Chen

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Figure 5

Pretreatment with the anti-FGL1 mAb slows the growth of liver metastatic and orthotopic tumors.

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Pretreatment with the anti-FGL1 mAb slows the growth of liver metastatic...
(A) Experimental protocol for the CRC liver metastasis model used in B and C. WT mice were injected intraperitoneally (i.p.) with 200 μg anti-FGL1 mAb or control rat IgG once every 4 days 4 times, starting 1 day before tumor cell challenge. On day 0, 2 × 105 MC38 tumor cells were intrasplenically (i.s.) challenged. On day 21 after challenge, the livers were harvested. (B) Representative photograph of livers. Bar, 1 cm. (C) Number of liver tumor nodules (n = 5/group). (D) Experimental protocol for the orthotopic liver cancer model used in E and F. WT mice were injected intraperitoneally (i.p.) with 200 μg anti-FGL1 mAb or control rat IgG once every 4 days 4 times, starting 1 day before tumor cell challenge. On day 0, 3 × 106 Hepa1-6 tumor cells were orthotopically challenged. (E) Representative photograph of livers. Bar, 1 cm. (F) Mean tumor diameter (n = 12 for the rat IgG group; n = 11 for the anti-FGL1 group) 15 days after challenge. Data are representative of 2 independent experiments (C) and pooled from 2 independent experiments (F). Each symbol (C and F) represents an individual mouse. Comparisons were performed by using 2-tailed unpaired Student’s t test (C and F). Data are presented as the mean ± SEM (C and F). **P < 0.01.