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Literature DB >> 34297917

Single-cell analysis defines a pancreatic fibroblast lineage that supports anti-tumor immunity.

Colin Hutton¹, Felix Heider¹, Adrian Blanco-Gomez¹, Antonia Banyard², Alexander Kononov¹, Xiaohong Zhang¹, Saadia Karim³, Viola Paulus-Hock³, Dale Watt³, Nina Steele⁴, Samantha Kemp⁵, Elizabeth K J Hogg¹, Joanna Kelly¹, Rene-Filip Jackstadt³, Filipa Lopes⁶, Matteo Menotti⁷, Luke Chisholm⁸, Angela Lamarca⁹, Juan Valle¹⁰, Owen J Sansom¹¹, Caroline Springer⁶, Angeliki Malliri⁷, Richard Marais⁸, Marina Pasca di Magliano¹², Santiago Zelenay¹³, Jennifer P Morton¹¹, Claus Jørgensen¹⁴.

Abstract

Fibroblasts display extensive transcriptional heterogeneity, yet functional annotation and characterization of their heterocellular relationships remains incomplete. Using mass cytometry, we chart the stromal composition of 18 murine tissues and 5 spontaneous tumor models, with an emphasis on mesenchymal phenotypes. This analysis reveals extensive stromal heterogeneity across tissues and tumors, and identifies coordinated relationships between mesenchymal and immune cell subsets in pancreatic ductal adenocarcinoma. Expression of CD105 demarks two stable and functionally distinct pancreatic fibroblast lineages, which are also identified in murine and human healthy tissues and tumors. Whereas CD105-positive pancreatic fibroblasts are permissive for tumor growth in vivo, CD105-negative fibroblasts are highly tumor suppressive. This restrictive effect is entirely dependent on functional adaptive immunity. Collectively, these results reveal two functionally distinct pancreatic fibroblast lineages and highlight the importance of mesenchymal and immune cell interactions in restricting tumor growth.

Entities: Chemical

Keywords: CAF; CD105; CyTOF; Eng; cancer-associated fibroblast lineages; mass cytometry; pancreatic cancer; tumor microenvironment; tumor-restrictive fibroblasts

Mesh：

Substances：

Year: 2021 PMID： 34297917 PMCID： PMC8443274 DOI： 10.1016/j.ccell.2021.06.017

Source DB: PubMed Journal: Cancer Cell ISSN： 1535-6108 Impact factor: 31.743

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