Immunotherapy reverses glioma-driven dysfunction of immune system homeostasis.
B DiVita DeanTyler WildesJoseph DeanOleg YegorovChanglin YangDavid ShinConnor FrancisJohn W FiggMathew SebastianLaura Falceto FontDan JinAlexandra ReidGinger MooreBrandon FernandezBrandon WummerCarmelle KuizonDuane MitchellCatherine T FloresPublished in: Journal for immunotherapy of cancer (2023)
Using scRNAseq, we observed an altered HSPC landscape in glioma-bearing versus non-tumor-bearing mice . In addition, an expansion of myeloid lineage subsets, including granulocyte macrophage precursors (GMPs) and MDSCs, were observed in glioma-bearing mice relative to non-tumor-bearing controls. Furthermore, MDSCs from glioma-bearing mice demonstrated increased suppressive capacity toward tumor-specific T cells as compared with MDSCs from non-tumor-bearing hosts. Interestingly, treatment with ACT overcame these suppressive properties. When HSPCs from glioma-bearing mice were transferred in the context of ACT, we observed significant survival benefit and long-term cures in orthotopic glioma models compared with mice treated with ACT using non-glioma-bearing HSPCs.