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. 2021 Apr;24(4):595-610.
doi: 10.1038/s41593-020-00789-y. Epub 2021 Mar 29.

Single-cell profiling of myeloid cells in glioblastoma across species and disease stage reveals macrophage competition and specialization

Ana Rita Pombo Antunes #  1   2 Isabelle Scheyltjens #  1   2 Francesca Lodi  3   4 Julie Messiaen  5 Asier Antoranz  5 Johnny Duerinck  6 Daliya Kancheva  7 Liesbet Martens  8   9   10 Karen De Vlaminck  1   2 Hannah Van Hove  1   2 Signe Schmidt Kjølner Hansen  1   2 Francesca Maria Bosisio  11 Koen Van der Borght  7 Steven De Vleeschouwer  12   13 Raf Sciot  11 Luc Bouwens  14 Michiel Verfaillie  15 Niels Vandamme  16   17 Roosmarijn E Vandenbroucke  18   9 Olivier De Wever  19   20 Yvan Saeys  16   17 Martin Guilliams  8   9 Conny Gysemans  21 Bart Neyns  22 Frederik De Smet  5 Diether Lambrechts  3   4 Jo A Van Ginderachter  1   2 Kiavash Movahedi  23   24
Affiliations

Single-cell profiling of myeloid cells in glioblastoma across species and disease stage reveals macrophage competition and specialization

Ana Rita Pombo Antunes et al. Nat Neurosci. 2021 Apr.

Abstract

Glioblastomas are aggressive primary brain cancers that recur as therapy-resistant tumors. Myeloid cells control glioblastoma malignancy, but their dynamics during disease progression remain poorly understood. Here, we employed single-cell RNA sequencing and CITE-seq to map the glioblastoma immune landscape in mouse tumors and in patients with newly diagnosed disease or recurrence. This revealed a large and diverse myeloid compartment, with dendritic cell and macrophage populations that were conserved across species and dynamic across disease stages. Tumor-associated macrophages (TAMs) consisted of microglia- or monocyte-derived populations, with both exhibiting additional heterogeneity, including subsets with conserved lipid and hypoxic signatures. Microglia- and monocyte-derived TAMs were self-renewing populations that competed for space and could be depleted via CSF1R blockade. Microglia-derived TAMs were predominant in newly diagnosed tumors, but were outnumbered by monocyte-derived TAMs following recurrence, especially in hypoxic tumor environments. Our results unravel the glioblastoma myeloid landscape and provide a framework for future therapeutic interventions.

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