| Literature DB >> 35063085 |
Hugo Gonzalez1, Wenbin Mei2, Isabella Robles2, Catharina Hagerling3, Breanna M Allen4, Trine Line Hauge Okholm5, Ankitha Nanjaraj2, Tamara Verbeek2, Sandhya Kalavacherla2, Merel van Gogh2, Stephen Georgiou2, Mariza Daras6, Joanna J Phillips7, Matthew H Spitzer8, Jeroen P Roose9, Zena Werb10.
Abstract
Brain metastasis (BrM) is the most common form of brain cancer, characterized by neurologic disability and an abysmal prognosis. Unfortunately, our understanding of the biology underlying human BrMs remains rudimentary. Here, we present an integrative analysis of >100,000 malignant and non-malignant cells from 15 human parenchymal BrMs, generated by single-cell transcriptomics, mass cytometry, and complemented with mouse model- and in silico approaches. We interrogated the composition of BrM niches, molecularly defined the blood-tumor interface, and revealed stromal immunosuppressive states enriched with infiltrated T cells and macrophages. Specific single-cell interrogation of metastatic tumor cells provides a framework of 8 functional cell programs that coexist or anticorrelate. Collectively, these programs delineate two functional BrM archetypes, one proliferative and the other inflammatory, that are evidently shaped through tumor-immune interactions. Our resource provides a foundation to understand the molecular basis of BrM in patients with tumor cell-intrinsic and host environmental traits.Entities:
Keywords: CyTOF; blood tumor barrier; human metastasis; metastasis-associated macrophages; metastasis-infiltrated T cells; metastatic niche; metastatic program; metastatic tumor cells; metastatic tumors; single cell
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Year: 2022 PMID: 35063085 PMCID: PMC8857062 DOI: 10.1016/j.cell.2021.12.043
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582