Genome Medicine (May 2021)

Single-cell characterization of macrophages in glioblastoma reveals MARCO as a mesenchymal pro-tumor marker

  • Andrew X. Chen,
  • Robyn D. Gartrell,
  • Junfei Zhao,
  • Pavan S. Upadhyayula,
  • Wenting Zhao,
  • Jinzhou Yuan,
  • Hanna E. Minns,
  • Athanassios Dovas,
  • Jeffrey N. Bruce,
  • Anna Lasorella,
  • Antonio Iavarone,
  • Peter Canoll,
  • Peter A. Sims,
  • Raul Rabadan

DOI
https://doi.org/10.1186/s13073-021-00906-x
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 13

Abstract

Read online

Abstract Background Macrophages are the most common infiltrating immune cells in gliomas and play a wide variety of pro-tumor and anti-tumor roles. However, the different subpopulations of macrophages and their effects on the tumor microenvironment remain poorly understood. Methods We combined new and previously published single-cell RNA-seq data from 98,015 single cells from a total of 66 gliomas to profile 19,331 individual macrophages. Results Unsupervised clustering revealed a pro-tumor subpopulation of bone marrow-derived macrophages characterized by the scavenger receptor MARCO, which is almost exclusively found in IDH1-wild-type glioblastomas. Previous studies have implicated MARCO as an unfavorable marker in melanoma and non-small cell lung cancer; here, we find that bulk MARCO expression is associated with worse prognosis and mesenchymal subtype. Furthermore, MARCO expression is significantly altered over the course of treatment with anti-PD1 checkpoint inhibitors in a response-dependent manner, which we validate with immunofluorescence imaging. Conclusions These findings illustrate a novel macrophage subpopulation that drives tumor progression in glioblastomas and suggest potential therapeutic targets to prevent their recruitment.

Keywords