Abstract
BACKGROUND: Pancreatic ductal adenocarcinoma (PDAC) is an aggressive malignancy with a poor survival rate, largely due to the lack of early diagnosis. Although myeloid cells are crucial in the tumour microenvironment, whether their specific subset can be a biomarker of PDAC progression is unclear. METHODS: We analysed IL-22 receptor expression in PDAC and peripheral blood. Additionally, we analysed gene expression profiles of IL-10R2(+)/IL-22R1(+) myeloid cells and the presence of these cells using single-cell RNA sequencing and murine orthotropic PDAC models, respectively, followed by examining the immunosuppressive function of IL-10R2(+)/IL-22R1(+) myeloid cells. Finally, the correlation between IL-10R2 expression and PDAC progression was evaluated. RESULTS: IL-10R2(+)/IL-22R1(+) myeloid cells were present in PDAC and peripheral blood. Blood IL-10R2(+) myeloid cells displayed a gene expression signature associated with tumour-educated circulating monocytes. IL-10R2(+)/IL-22R1(+) myeloid cells from human myeloid cell culture inhibited T cell proliferation. By mouse models for PDAC, we found a positive correlation between pancreatic tumour growth and increased blood IL-10R2(+)/IL-22R1(+) myeloid cells. IL-10R2(+)/IL-22R1(+) myeloid cells from an early phase of the PDAC model suppressed T cell proliferation and cytotoxicity. IL-10R2(+) myeloid cells indicated tumour recurrence 130 days sooner than CA19-9 in post-pancreatectomy patients. CONCLUSIONS: IL-10R2(+)/IL-22R1(+) myeloid cells in the peripheral blood might be an early marker of PDAC prognosis.