Glioblastoma genetic drivers dictate the function of tumor-associated macrophages/microglia and responses to CSF1R inhibition | Zendy

Rohit Rao | Zendy; Rong Han | Zendy; Sean Ogurek | Zendy; Chengbin Xue | Zendy; Lai Man Natalie Wu | Zendy; Liguo Zhang | Zendy; Li Zhang | Zendy; Jian Hu | Zendy; Timothy N. Phoenix | Zendy; Stephen N. Waggoner | Zendy; Q. Richard Lu | Zendy

Open Access

Glioblastoma genetic drivers dictate the function of tumor-associated macrophages/microglia and responses to CSF1R inhibition

Author(s) -

Rohit Rao,

Rong Han,

Sean Ogurek,

Chengbin Xue,

Lai Man Natalie Wu,

Liguo Zhang,

Li Zhang,

Jian Hu,

Timothy N. Phoenix,

Stephen N. Waggoner,

Q. Richard Lu

Publication year - 2021

Publication title -

neuro-oncology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 4.005

H-Index - 125

eISSN - 1523-5866

pISSN - 1522-8517

DOI - 10.1093/neuonc/noab228

Subject(s) - pdgfb , glioma , cancer research , mesenchymal stem cell , microglia , pdgfrb , tumor microenvironment , angiogenesis , stromal cell , biology , chemistry , microbiology and biotechnology , immunology , receptor , inflammation , growth factor , tumor cells , platelet derived growth factor receptor , gene , biochemistry

Background Tumor-associated macrophages/microglia (TAMs) are prominent microenvironment components in human glioblastoma (GBM) that are potential targets for anti-tumor therapy. However, TAM depletion by CSF1R inhibition showed mixed results in clinical trials. We hypothesized that GBM subtype-specific tumor microenvironment (TME) conveys distinct sensitivities to TAM targeting. Methods We generated syngeneic PDGFB- and RAS-driven GBM models that resemble proneural-like and mesenchymal-like gliomas, and determined the effect of TAM targeting by CSF1R inhibitor PLX3397 on glioma growth. We also investigated the co-targeting of TAMs and angiogenesis on PLX3397-resistant RAS-driven GBM. Using single-cell transcriptomic profiling, we further explored differences in TME cellular compositions and functions in PDGFB- and RAS-driven gliomas. Results We found that growth of PDGFB-driven tumors was markedly inhibited by PLX3397. In contrast, depletion of TAMs at the early phase accelerated RAS-driven tumor growth and had no effects on other proneural and mesenchymal GBM models. In addition, PLX3397-resistant RAS-driven tumors did not respond to PI3K signaling inhibition. Single-cell transcriptomic profiling revealed that PDGFB-driven gliomas induced expansion and activation of pro-tumor microglia, whereas TAMs in mesenchymal RAS-driven GBM were enriched in pro-inflammatory and angiogenic signaling. Co-targeting of TAMs and angiogenesis decreased cell proliferation and changed the morphology of RAS-driven gliomas. Conclusions Our work identifies functionally distinct TAM subpopulations in the growth of different glioma subtypes. Notably, we uncover a potential responsiveness of resistant mesenchymal-like gliomas to combined anti-angiogenic therapy and CSF1R inhibition. These data highlight the importance of characterization of the microenvironment landscape in order to optimally stratify patients for TAM-targeted therapy.

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