S1PR1-STAT3 Signaling Is Crucial for Myeloid Cell Colonization at Future Metastatic Sites

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• 作者：Jiehui Dengp>1p> ; Yong Liup>1p> ; Heehyoung Leep>1p> ; Andreas Herrmannp>1p> ; Wang Zhangp>1p> ; Chunyan Zhangp>1p> ; Shudan Shenp>1p> ; Saul  ; J. Pricemanp>1p> ; Maciej Kujawskip>1p> ; Sumanta  ; K. Palp>2p> ; Andrew Raubitschekp>1p> ; Dave  ; S.B. Hoonp>5p> ; Stephen Formanp>3p> ; Robert  ; A. Figlinp>6p> ; Jie Liup>7p>p> ; p>p>8p> ; Richard Jovep>4p> ; Hua Yup>1p>p> ; p>p>8p>p> ; p>p>hyu@coh.orgp>
• 刊名：Cancer Cell
• 出版年：2012
• 期刊代码：43_15356108
• 类别：med
• 出版时间：15 May, 2012
• 卷：21
• 期：5
• 页码：642-654
• 文件大小：2086 K

摘要

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Summary

Recent studies underscore the importance of myeloid cells in rendering distant organs hospitable for disseminating tumor cells to colonize. However, what enables myeloid cells to have an apparently superior capacity to colonize distant organs is unclear. Here, we show that S1PR1-STAT3 upregulation in tumor cells induces factors that activate S1PR1-STAT3 in various cells in premetastatic sites, leading to premetastatic niche formation. Targeting either S1PR1 or STAT3 in myeloid cells disrupts existing premetastatic niches. S1PR1-STAT3 pathway enables myeloid cells to intravasate, prime the distant organ microenvironment and mediate sustained proliferation and survival of their own and other stromal cells at future metastatic sites. Analyzing tumor-free lymph nodes from cancer patients shows elevated myeloid infiltrates, STAT3 activity, and increased survival signal.