Myeloid activation clears ascites and reveals IL27-dependent regression of metastatic ovarian cancer

髓系细胞活化可清除腹水并揭示IL27依赖性的转移性卵巢癌消退

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作者:Brennah Murphy # ,Taito Miyamoto # ,Bryan S Manning ,Gauri Mirji ,Alessio Ugolini ,Toshitha Kannan ,Kohei Hamada ,Yanfang P Zhu ,Daniel T Claiborne ,Lu Huang ,Rugang Zhang ,Yulia Nefedova ,Andrew Kossenkov ,Filippo Veglia ,Rahul Shinde ,Nan Zhang

Abstract

Patients with metastatic ovarian cancer (OvCa) have a 5-year survival rate of <30% due to the persisting dissemination of chemoresistant cells in the peritoneal fluid and the immunosuppressive microenvironment in the peritoneal cavity. Here, we report that intraperitoneal administration of β-glucan and IFNγ (BI) induced robust tumor regression in clinically relevant models of metastatic OvCa. BI induced tumor regression by controlling fluid tumor burden and activating localized antitumor immunity. β-glucan alone cleared ascites and eliminated fluid tumor cells by inducing intraperitoneal clotting in the fluid and Dectin-1-Syk-dependent NETosis in the omentum. In omentum tumors, BI expanded a novel subset of immunostimulatory IL27+ macrophages and neutralizing IL27 impaired BI efficacy in vivo. Moreover, BI directly induced IL27 secretion in macrophages where single agent treatment did not. Finally, BI extended mouse survival in a chemoresistant model and significantly improved chemotherapy response in a chemo-sensitive model. In summary, we propose a new therapeutic strategy for the treatment of metastatic OvCa.

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