Tumor-associated macrophages (TAMs) are strongly associated with poor survival in neuroblastomas that lack MYCN amplification. To study TAM action in neuroblastomas, we used a novel murine model of spontaneous neuroblastoma lacking MYCN amplification, and observed recruitment and polarization of TAMs, which in turn enhanced neuroblastoma proliferation and growth. In both murine and human neuroblastoma cells, we found that TAMs increased STAT3 activation in neuroblastoma cells and transcriptionally up-regulated the MYC oncogene. Analysis of human neuroblastoma tumor specimens revealed that MYC up-regulation correlates with markers of TAM infiltration. In an IL6(ko) neuroblastoma model, the absence of IL-6 protein had no effect on tumor development and prevented neither STAT3 activation nor MYC up-regulation. In contrast, inhibition of JAK-STAT activation using AZD1480 or the clinically admissible inhibitor ruxolitinib significantly reduced TAM-mediated growth of neuroblastomas implanted subcutaneously in NOD scid gamma mice. Our results point to a unique mechanism in which TAMs promote tumor cells that lack amplification of an oncogene common to the malignancy by up-regulating transcriptional expression of a distinct oncogene from the same gene family, and underscore the role of IL-6-independent activation of STAT3 in this mechanism. Amplification of MYCN or constitutive up-regulation of MYC protein is observed in approximately half of high-risk tumors; our findings indicate a novel role of TAMs as inducers of MYC expression in neuroblastomas lacking independent oncogene activation.
Tumor-associated macrophages promote neuroblastoma via STAT3 phosphorylation and up-regulation of c-MYC
肿瘤相关巨噬细胞通过 STAT3 磷酸化和 c-MYC 上调促进神经母细胞瘤
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作者:Michael D Hadjidaniel, Sakunthala Muthugounder, Long T Hung, Michael A Sheard, Soheila Shirinbak, Randall Y Chan, Rie Nakata, Lucia Borriello, Jemily Malvar, Rebekah J Kennedy, Hiroshi Iwakura, Takashi Akamizu, Richard Sposto, Hiroyuki Shimada, Yves A DeClerck, Shahab Asgharzadeh
| 期刊: | Oncotarget | 影响因子: | 0.000 |
| 时间: | 2017 | 起止号: | 2017 Sep 16;8(53):91516-91529. |
| doi: | 10.18632/oncotarget.21066 | 研究方向: | 神经、肿瘤、表观遗传 |
| 细胞类型: | 巨噬细胞 | ||
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