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KMID : 0620920200520121976
Experimental & Molecular Medicine
2020 Volume.52 No. 12 p.1976 ~ p.1988
Tumor-promoting macrophages prevail in malignant ascites of advanced gastric cancer
Eum Hye-Hyeon

Kwon Min-Suk
Ryu Da-Eun
Jo A-Reum
Chung Woo-Sung
Kim Na-Young
Hong You-Rae
Son Dae-Soon
Kim Seung-Tae
Lee Jee-Yun
Lee Hae-Ock
Park Woong-Yang
Abstract
Gastric cancer (GC) patients develop malignant ascites as the disease progresses owing to peritoneal metastasis. GC patients with malignant ascites have a rapidly deteriorating clinical course with short survival following the onset of malignant ascites. Better optimized treatment strategies for this subset of patients are needed. To define the cellular characteristics of malignant ascites of GC, we used single-cell RNA sequencing to characterize tumor cells and tumor-associated macrophages (TAMs) from four samples of malignant ascites and one sample of cerebrospinal fluid. Reference transcriptomes for M1 and M2 macrophages were generated by in vitro differentiation of healthy blood-derived monocytes and applied to assess the inflammatory properties of TAMs. We analyzed 180 cells, including tumor cells, macrophages, and mesothelial cells. Dynamic exchange of tumor-promoting signals, including the CCL3?CCR1 or IL1B?IL1R2 interactions, suggests macrophage recruitment and anti-inflammatory tuning by tumor cells. By comparing these data with reference transcriptomes for M1-type and M2-type macrophages, we found noninflammatory characteristics in macrophages recovered from the malignant ascites of GC. Using public datasets, we demonstrated that the single-cell transcriptome-driven M2-specific signature was associated with poor prognosis in GC. Our data indicate that the anti-inflammatory characteristics of TAMs are controlled by tumor cells and present implications for treatment strategies for GC patients in which combination treatment targeting cancer cells and macrophages may have a reciprocal synergistic effect.
KEYWORD
Cancer genomics, Gastric cancer, RNA sequencing
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