期刊
MOLECULAR CANCER THERAPEUTICS
卷 14, 期 6, 页码 1385-1394出版社
AMER ASSOC CANCER RESEARCH
DOI: 10.1158/1535-7163.MCT-14-0969
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资金
- European Research Council (under FP-7 program) [260633]
- Israel Science Foundation [490/12]
- Israel Cancer Research Fund [708/12]
- Rappaport funds
- Miriam and Aaron Gutwirth Studentship
- European Research Council (ERC) [260633] Funding Source: European Research Council (ERC)
Acquired resistance to therapy is a major obstacle in clinical oncology, and little is known about the contributing mechanisms of the host response to therapy. Here, we show that the proinflammatory cytokine IL1 beta is overexpressed in response to paclitaxel chemotherapy in macrophages, subsequently promoting the invasive properties of malignant cells. In accordance, blocking IL1 beta, or its receptor, using either genetic or pharmacologic approach, results in slight retardation of primary tumor growth; however, it accelerates metastasis spread. Tumors from mice treated with combined therapy of paclitaxel and the IL1 receptor antagonist anakinra exhibit increased number of M2 macrophages and vessel leakiness when compared with paclitaxel monotherapy-treated mice, indicating a prometastatic role of M2 macrophages in the IL1 beta-deprived microenvironment. Taken together, these findings demonstrate the dual effects of blocking the IL1 pathway on tumor growth. Accordingly, treatments using add-on drugs to conventional therapy should be investigated in appropriate tumor models consisting of primary tumors and their metastases. (C) 2015 AACR.
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