Macrophages reprogramming improves immunotherapy of IL-33 in peritoneal metastasis of gastric cancer

Author:

Che KeyingORCID,Luo Yuting,Song Xueru,Yang Zhe,Wang Hanbing,Shi TaoORCID,Wang Yue,Wang Xuan,Wu Hongyan,Yu Lixia,Liu Baorui,Wei JiaORCID

Abstract

AbstractPeritoneal metastasis (PM) has a suppressive tumor immune microenvironment (TIME) that limits the effects of immunotherapy. This study aimed to investigate the immunomodulatory effects of intraperitoneal administration of IL-33, a cytokine that is reported to potentiate antitumor immunity and inhibit metastasis. We found survival was significantly prolonged in patients with high IL-33 mRNA expression. In immunocompetent mice, intraperitoneal administration of IL-33 could induce a celiac inflammatory environment, activate immunologic effector cells, and reverse the immunosuppressive tumor microenvironment, which effectively delayed tumor progression and PM of gastric cancer. Mechanistically, IL-33 could induce M2 polarization by activating p38-GATA-binding protein 3 signaling. IL-33 combined with anti-CSF1R or p38 inhibitor to regulate tumor-associated macrophages (TAMs) had a synergistic antitumor effect. Inducing a local inflammatory milieu by IL-33 administration provided a novel approach for treating peritoneal metastasis, which, when combined with TAM reprogramming to reshape TIME, can achieve better treatment efficacy.

Funder

Funder for Distinguished Young Scholars of Jiangsu Province

Fundermental Research Funds for the Central Universities

Incubation Fundation of Shandong Provincial Hospital

Shandong Provincial Natural Science Foundation

Publisher

Springer Science and Business Media LLC

Subject

Molecular Medicine

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