CD206 Modulates the Role of M2 Macrophages in the Origin of Metastatic Tumors

Overview

Journal J Cancer

Specialty Oncology

Date 2024 Feb 15

PMID 38356723

Authors

Hui Li

Ying-Qi Miao

Li-Ping Suo

Xi Wang

Yi-Qing Mao

Xue-Hui Zhang

Na Zhou

Jun-Rui Tian

Xiu-Yan Yu

Tong-Xia Wang

Yan Gao

Hong-Yan Guo

Zheng Zhang

Dian-Sheng Ma

Hong-Xia Wu

Yan-Wei Cui

Xi-Liang Zhang

Xiao-Chun Chi

Yu-Chi Li

David M Irwin

Gang Niu

Huan-Ran Tan

Affiliations

Soon will be listed here.

Abstract

Tumor metastasis is a key factor affecting the life of patients with malignant tumors. For the past hundred years, scientists have focused on how to kill cancer cells and inhibit their metastasis , but few breakthroughs have been made. Here we hypothesized a novel mode for cancer metastasis. We show that the phagocytosis of apoptotic tumor cells by macrophages leads to their polarization into the M2 phenotype, and that the expression of stem cell related as well as drug resistance related genes was induced. Therefore, it appears that M2 macrophages have "defected" and have been transformed into the initial "metastatic cancer cells", and thus are the source, at least in part, of the distal tissue tumor metastasis. This assumption is supported by the presence of fused cells with characteristics of both macrophage and tumor cell observed in the peripheral blood and ascites of patients with ovarian cancer. By eliminating the expression of CD206 in M2 macrophages using siRNA, we show that the growth and metastasis of tumors was suppressed using both cell line and with experimental mouse models. In summary, we show that M2 macrophages in the blood circulation underwent a "change of loyalty" to become "cancer cells" that transformed into distal tissue metastasis, which could be suppressed by the knockdown of CD206 expression.

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