| Literature DB >> 30343900 |
Matthew M Gubin1, Ekaterina Esaulova2, Jeffrey P Ward3, Olga N Malkova4, Daniele Runci1, Pamela Wong5, Takuro Noguchi6, Cora D Arthur1, Wei Meng1, Elise Alspach1, Ruan F V Medrano1, Catrina Fronick7, Michael Fehlings8, Evan W Newell8, Robert S Fulton7, Kathleen C F Sheehan1, Stephen T Oh9, Robert D Schreiber10, Maxim N Artyomov11.
Abstract
Although current immune-checkpoint therapy (ICT) mainly targets lymphoid cells, it is associated with a broader remodeling of the tumor micro-environment. Here, using complementary forms of high-dimensional profiling, we define differences across all hematopoietic cells from syngeneic mouse tumors during unrestrained tumor growth or effective ICT. Unbiased assessment of gene expression of tumor-infiltrating cells by single-cell RNA sequencing (scRNAseq) and longitudinal assessment of cellular protein expression by mass cytometry (CyTOF) revealed significant remodeling of both the lymphoid and myeloid intratumoral compartments. Surprisingly, we observed multiple subpopulations of monocytes/macrophages, distinguishable by the markers CD206, CX3CR1, CD1d, and iNOS, that change over time during ICT in a manner partially dependent on IFNγ. Our data support the hypothesis that this macrophage polarization/activation results from effects on circulatory monocytes and early macrophages entering tumors, rather than on pre-polarized mature intratumoral macrophages.Entities:
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Year: 2018 PMID: 30343900 PMCID: PMC6501221 DOI: 10.1016/j.cell.2018.09.030
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582