The influence of myeloid‐derived suppressor cells on angiogenesis and tumor growth after cancer surgery

血管生成 髓源性抑制细胞 癌症研究 医学 CD33 转移 肺癌 肺癌手术 人口 新生血管 免疫学 围手术期 骨髓 癌症 病理 抑制器 内科学 干细胞 生物 外科 环境卫生 川地34 遗传学
作者
Jun Wang,Xiaosan Su,Yang Liu,Fei Qiao,Fang Yu,Lu Yu,Qian Yang,Yiyin Wang,Yanfeng Yin,Rui Chen,Zhipeng Hong
出处
期刊:International Journal of Cancer [Wiley]
卷期号:138 (11): 2688-2699 被引量:48
标识
DOI:10.1002/ijc.29998
摘要

While myeloid‐derived suppressor cells (MDSCs) have been reported to participate in the promotion of angiogenesis and tumor growth, little is known about their presence and function during perioperative period. Here, we demonstrated that human MDSCs expressing CD11b + , CD33 + and HLA‐DR – significantly increased in lung cancer patients after thoracotomy. CD11b + CD33 + HLA‐DR – MDSCs isolated 24 hr after surgery from lung cancer patients were more efficient in promoting angiogenesis and tumor growth than MDSCs isolated before surgical operation in allograft tumor model. In addition, CD11b + CD33 + HLA‐DR – MDSCs produced high levels of MMP‐9. Using an experimental lung metastasis mouse model, we demonstrated that the numbers of metastases on lung surface and Gr‐1 + CD11b + MDSCs at postoperative period were enhanced in proportion to the degree of surgical manipulation. We also examined that syngeneic bone marrow mesenchymal stem cells (BMSCs) significantly inhibited the induction and proliferation of Gr‐1 + CD11b + MDSCs and further prevented lung metastasis formation in the mice undergoing laparotomy. Taken together, our results suggest that postoperatively induced MDSCs were qualified with potent proangiogenic and tumor‐promotive ability and this cell population should be considered as a target for preventing postoperative tumor metastasis.

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