Single-cell RNA sequencing reveals evolution of immune landscape during glioblastoma progression

被引:0
|
作者
Alan T. Yeo
Shruti Rawal
Bethany Delcuze
Anthos Christofides
Agata Atayde
Laura Strauss
Leonora Balaj
Vaughn A. Rogers
Erik J. Uhlmann
Hemant Varma
Bob S. Carter
Vassiliki A. Boussiotis
Al Charest
机构
[1] Beth Israel Deaconess Medical Center,Department of Medicine
[2] Harvard Medical School,Sackler School of Graduate Studies
[3] Tufts University School of Medicine,Department of Neurosurgery
[4] Massachusetts General Hospital,Department of Neurology
[5] Harvard Medical School,Department of Pathology
[6] Beth Israel Deaconess Medical Center,Cancer Research Institute
[7] Harvard Medical School,undefined
[8] Beth Israel Deaconess Medical Center,undefined
[9] Harvard Medical School,undefined
[10] Beth Israel Deaconess Medical Center,undefined
来源
Nature Immunology | 2022年 / 23卷
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摘要
Glioblastoma (GBM) is an incurable primary malignant brain cancer hallmarked with a substantial protumorigenic immune component. Knowledge of the GBM immune microenvironment during tumor evolution and standard of care treatments is limited. Using single-cell transcriptomics and flow cytometry, we unveiled large-scale comprehensive longitudinal changes in immune cell composition throughout tumor progression in an epidermal growth factor receptor-driven genetic mouse GBM model. We identified subsets of proinflammatory microglia in developing GBMs and anti-inflammatory macrophages and protumorigenic myeloid-derived suppressors cells in end-stage tumors, an evolution that parallels breakdown of the blood–brain barrier and extensive growth of epidermal growth factor receptor+ GBM cells. A similar relationship was found between microglia and macrophages in patient biopsies of low-grade glioma and GBM. Temozolomide decreased the accumulation of myeloid-derived suppressor cells, whereas concomitant temozolomide irradiation increased intratumoral GranzymeB+ CD8+T cells but also increased CD4+ regulatory T cells. These results provide a comprehensive and unbiased immune cellular landscape and its evolutionary changes during GBM progression.
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页码:971 / 984
页数:13
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