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Publication : Disease-specific suppressive granulocytes participate in glioma progression.

First Author  Zhao J Year  2024
Journal  Cell Rep Volume  43
Issue  12 Pages  115014
PubMed ID  39630582 Mgi Jnum  J:361369
Mgi Id  MGI:7852053 Doi  10.1016/j.celrep.2024.115014
Citation  Zhao J, et al. (2024) Disease-specific suppressive granulocytes participate in glioma progression. Cell Rep 43(12):115014
abstractText  Glioblastoma represents one of the most aggressive cancers, characterized by severely limited therapeutic options. Despite extensive investigations into this brain malignancy, cellular and molecular components governing its immunosuppressive microenvironment remain incompletely understood. Here, we identify a distinct neutrophil subpopulation, termed disease-specific suppressive granulocytes (DSSGs), present in human glioblastoma and lower-grade gliomas. DSSGs exhibit the concurrent expression of multiple immunosuppressive and immunomodulatory signals, and their abundance strongly correlates with glioma grades and poor clinical outcomes. Genetic disruption of neutrophil recruitment in immunocompetent mouse models of gliomas, achieved through Cxcl1 knockout in glioma cells or host-specific Cxcr2 deletion or diphtheria toxin A-mediated neutrophil depletion, can significantly enhance antitumor immunity and prolong survival. Further, we reveal that the skull bone marrow and meninges can be the primary sources of neutrophils and DSSGs in human and mouse glioma tumors. These findings demonstrate a critical mechanism underlying the establishment of the immunosuppressive microenvironment in gliomas.
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