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  5. Fibrotic response to anti-CSF-1R therapy potentiates glioblastoma recurrence

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Article
en
2024

Fibrotic response to anti-CSF-1R therapy potentiates glioblastoma recurrence

0 Datasets

0 Files

en
2024
Vol 42 (9)
Vol. 42
DOI: 10.1016/j.ccell.2024.08.012

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Douglas Hanahan
Douglas Hanahan

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Spencer S. Watson
Anoek Zomer
Nadine Fournier
+17 more

Abstract

Glioblastoma recurrence is currently inevitable despite extensive standard-of-care treatment. In preclinical studies, an alternative strategy of targeting tumor-associated macrophages and microglia through CSF-1R inhibition was previously found to regress established tumors and significantly increase overall survival. However, recurrences developed in ∼50% of mice in long-term studies, which were consistently associated with fibrotic scars. This fibrotic response is observed following multiple anti-glioma therapies in different preclinical models herein and in patient recurrence samples. Multi-omics analyses of the post-treatment tumor microenvironment identified fibrotic areas as pro-tumor survival niches that encapsulated surviving glioma cells, promoted dormancy, and inhibited immune surveillance. The fibrotic treatment response was mediated by perivascular-derived fibroblast-like cells via activation by transforming growth factor β (TGF-β) signaling and neuroinflammation. Concordantly, combinatorial inhibition of these pathways inhibited treatment-associated fibrosis, and significantly improved survival in preclinical trials of anti-colony-stimulating factor-1 receptor (CSF-1R) therapy.

How to cite this publication

Spencer S. Watson, Anoek Zomer, Nadine Fournier, João Lourenço, Manfredo Quadroni, Agnieszka Chryplewicz, Sina Nassiri, Pauline Aubel, Simona Avanthay, Davide Croci, Erik R. Abels, Marike L. D. Broekman, Douglas Hanahan, Jason T. Huse, Roy Thomas Daniel, Monika E. Hegi, Krisztián Homicskó, Giulia Cossu, Andreas F. Hottinger, Johanna A. Joyce (2024). Fibrotic response to anti-CSF-1R therapy potentiates glioblastoma recurrence. , 42(9), DOI: https://doi.org/10.1016/j.ccell.2024.08.012.

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Publication Details

Type

Article

Year

2024

Authors

20

Datasets

0

Total Files

0

Language

en

DOI

https://doi.org/10.1016/j.ccell.2024.08.012

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