Identification of novel myeloid-derived cell states with implication in cancer outcome

Author:

Guimarães Gabriela Rapozo,Maklouf Giovanna ReskORCID,Teixeira Cristiane EstevesORCID,de Oliveira Santos Leandro,Tessarollo Nayara Gusmão,Pretti Marco Antônio,Toledo Nayara Evelin,da Cruz Jéssica Gonçalves Vieira,Falchetti Marcelo,Dimas Mylla M.,Serain Alessandra Freitas,de Macedo Fabiane Carvalho,Rodrigues Fabiana Resende,Bastos Nina Carrossini,da Silva Jesse Lopes,da Rocha Edroaldo Lummertz,Chaves Cláudia Bessa Pereira,de Melo Andreia Cristina,Moraes-Vieira Pedro Manoel Mendes,Mori Marcelo A.,Boroni MarianaORCID

Abstract

AbstractTumor-associated myeloid-derived cells (MDCs) significantly impact cancer prognosis and treatment response due to their remarkable plasticity and tumorigenic behaviors. We integrated single-cell RNA-Sequencing datasets from seven different cancers, resulting in a comprehensive collection of 29 MDC subpopulations in the tumor microenvironment (TME). Distinguishing resident-tissue from monocyte-derived macrophages, we discovered a resident-tissue-like subpopulation within monocyte-derived macrophages. Additionally, hypoxia-driven macrophages emerged as a prominent TME component. Deconvolution of these profiles revealed five subpopulations as independent prognostic markers across various cancer types. Validation in large cohorts confirmed the FOLR2-expressing macrophage association with poor clinical outcomes in ovarian and triple-negative breast cancer. Moreover, the marker TREM2, commonly used to define immunosuppressive tumor-associated macrophages, cannot solely predict cancer prognosis, as different polarization states of macrophages express this marker in a context-dependent manner. This comprehensive MDC atlas offers valuable insights and a foundation for novel analyses, advancing strategies for treating solid cancers.

Publisher

Cold Spring Harbor Laboratory

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