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10.1158/2159-8290.CD-15-1157

http://scihub22266oqcxt.onion/10.1158/2159-8290.CD-15-1157
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suck abstract from ncbi


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pmid27072748
      Cancer+Discov 2016 ; 6 (6 ): 630-49
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  • Neutrophils Suppress Intraluminal NK Cell-Mediated Tumor Cell Clearance and Enhance Extravasation of Disseminated Carcinoma Cells #MMPMID27072748
  • Spiegel A ; Brooks MW ; Houshyar S ; Reinhardt F ; Ardolino M ; Fessler E ; Chen MB ; Krall JA ; DeCock J ; Zervantonakis IK ; Iannello A ; Iwamoto Y ; Cortez-Retamozo V ; Kamm RD ; Pittet MJ ; Raulet DH ; Weinberg RA
  • Cancer Discov 2016[Jun]; 6 (6 ): 630-49 PMID27072748 show ga
  • Immune cells promote the initial metastatic dissemination of carcinoma cells from primary tumors. In contrast to their well-studied functions in the initial stages of metastasis, the specific roles of immunocytes in facilitating progression through the critical later steps of the invasion-metastasis cascade remain poorly understood. Here, we define novel functions of neutrophils in promoting intraluminal survival and extravasation at sites of metastatic dissemination. We show that CD11b(+)/Ly6G(+) neutrophils enhance metastasis formation via two distinct mechanisms. First, neutrophils inhibit natural killer cell function, which leads to a significant increase in the intraluminal survival time of tumor cells. Thereafter, neutrophils operate to facilitate extravasation of tumor cells through the secretion of IL1? and matrix metalloproteinases. These results identify neutrophils as key regulators of intraluminal survival and extravasation through their cross-talk with host cells and disseminating carcinoma cells. SIGNIFICANCE: This study provides important insights into the systemic contributions of neutrophils to cancer metastasis by identifying how neutrophils facilitate intermediate steps of the invasion-metastasis cascade. We demonstrate that neutrophils suppress natural killer cell activity and increase extravasation of tumor cells. Cancer Discov; 6(6); 630-49. ©2016 AACR.This article is highlighted in the In This Issue feature, p. 561.
  • |Adoptive Transfer [MESH]
  • |Animals [MESH]
  • |Biomarkers [MESH]
  • |Carcinoma/genetics/*immunology/metabolism/*pathology [MESH]
  • |Cell Communication [MESH]
  • |Cell Line, Tumor [MESH]
  • |Cell Movement [MESH]
  • |Cell Survival [MESH]
  • |Cytokines/biosynthesis [MESH]
  • |Disease Models, Animal [MESH]
  • |Endothelial Cells/metabolism [MESH]
  • |Heterografts [MESH]
  • |Humans [MESH]
  • |Immunity, Innate [MESH]
  • |Immunophenotyping [MESH]
  • |Killer Cells, Natural/*immunology/metabolism [MESH]
  • |Matrix Metalloproteinases/metabolism [MESH]
  • |Mice [MESH]
  • |Mice, Knockout [MESH]
  • |Neoplasm Invasiveness [MESH]
  • |Neoplasm Metastasis [MESH]
  • |Neutrophils/*immunology/metabolism [MESH]


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