High-dimensional immunotyping of tumors grown in obese and non-obese mice
Author(s) -
Cara E Wogsland,
Hilde E. Lien,
Line Pedersen,
Pahul Hanjra,
Sturla Magnus Grøndal,
Rolf A. Brekken,
James B. Lorens,
Nils Halberg
Publication year - 2021
Publication title -
disease models and mechanisms
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.327
H-Index - 83
eISSN - 1754-8411
pISSN - 1754-8403
DOI - 10.1242/dmm.048977
Subject(s) - immune system , mass cytometry , biology , cd8 , breast cancer , disease , cancer , inflammation , multicellular organism , flow cytometry , immunology , obesity , cancer research , tumor microenvironment , cell , medicine , endocrinology , phenotype , genetics , gene
Obesity is a disease characterized by chronic low-grade systemic inflammation and has been causally linked to the development of 13 cancer types. Several studies have been undertaken to determine whether tumors evolving in obese environments adapt differential interactions with immune cells and whether this can be connected to disease outcome. Most of these studies have been limited to single-cell lines and tumor models and analysis of limited immune cell populations. Given the multicellular complexity of the immune system and its dysregulation in obesity, we applied high-dimensional suspension mass cytometry to investigate how obesity affects tumor immunity. We used a 36-marker immune-focused mass cytometry panel to interrogate the immune landscape of orthotopic syngeneic mouse models of pancreatic and breast cancer. Unanchored batch correction was implemented to enable simultaneous analysis of tumor cohorts to uncover the immunotypes of each cancer model and reveal remarkably model-specific immune regulation. In the E0771 breast cancer model, we demonstrate an important link to obesity with an increase in two T-cell-suppressive cell types and a decrease in CD8 T cells.
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