PO.IM01.01 · 免疫学
Biphasic, time-dependent neutrophil biology in glioblastoma revealed by in vivo survival and flow cytometry with single-cell transcriptomic corroboration
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摘要 Abstract
Introduction: Tumor-associated neutrophils (TANs) are abundant in glioblastoma (GBM), yet their functions are phase-dependent. We investigated whether TANs are differentially transcribed from peripheral blood neutrophils (PBNs), if they acquire antigen-presenting functions in situ, and if neutrophil depletion timing influences survival and intratumoral immunity
Methods: Transcriptomics: Integrated analysis of publicly deposited recent human GBM data sets (bulk RNA-seq and scRNA-seq; Seurat standard pipeline, stringent QC, integration/UMAP, Wilcoxon DE). Prespecified modules: co-stimulation (CD83/CD86/CD40/ICOSLG), MHC-II (HLA-DRB3/A, DPA1/DPB1), and antigen-processing/chaperones (CD74, CALR, PSME2, HLA-DMA/DMB).
In vivo survival: Orthotopic CT2A and GL261; anti-Ly6G (1A8) or isotype on two schedules, (day −1 pre-implantation through ≥day 14) and delayed (start day +8). Kaplan-Meier/log-rank; Cox models (HR, 95% CI).
Ex vivo flow (day 8): Bead-normalized spectral cytometry; CD45+ leukocytes; CD11b+ myeloids (Ly6G+ neutrophils; Ly6C^hi monocytes), F4/80+ TAMs with MHC-II, CD3+/CD8+ T cells. Two-sided Mann-Whitney; FDR where indicated. Ly6G epitope masking identified; depletion confirmed by CD11b+SSC^hi back-gating and weekly blood counts.
Results: Transcriptomics: TANs vs PBNs showed coherent upregulation of APC/co-stimulatory programs (CD83/CD86/CD40/ICOSLG; HLA-DR/DP; CD74/CALR/PSME2/HLA-DMA/DMB), in line with dendritic-like, non-cytotoxic TAN states.
Survival (biphasic): Previous anti-Ly6G impaired outcomes, CT2A (n=9/arm) median 17 vs 23 days; HR 1.95 (1.10-3.46), p=0.018. Subsequent depletion abrogated this penalty, CT2A HR 1.23 (0.68-2.22), p=0.49;
Flow (day 8): Early-depleted tumors contained more Ly6C^hi monocytes (of CD45+: 29% vs 18%, p=0.006), fewer CD8+ T cells (3.2% vs 6.1%, p=0.011), and lower CD8:Ly6C^hi ratio (0.11 vs 0.36, p=0.004). Directional but non-significant aggregates: CD11b+ myeloids (68% vs 55%, p=0.07), CD3+T cells (9% vs 14%, p=0.09), reduced MHC-II on F4/80+ TAMs (p=0.08), reduced CD11c⁺MHC-II^hi APCs (q≈0.12).
Conclusion: Human TANs take up APC/co-stimulatory programs, and timing is critical: pre-implantation neutrophil depletion imposes a myeloid-skewed, antigen-poor, T-cell-depleted setting, augments survival, while late targeting diminishes this. These observations favor phase-specific TAN modulation. maintenance or re-education of early TANs and suppression of late suppressive programs selectively, to regulate biomarker-based GBM immunotherapies.
利益披露 Disclosure
M. A. Abikenari, None..
J. Choi, None..
J. Liu, None..
A. Sjoholm, None..
G. Nageeb, None..
J. Poe, None..
A. Tran, None..
D. Bakalov, None..
R. Medikonda, None..
L. Kim, None..
C. Wu, None..
K. Cho, None..
M. Banu, None..
M. Lim, None.