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Tissues in different anatomical sites can sculpt and vary the tumor microenvironment to affect responses to therapy

journal contribution
posted on 2024-11-01, 22:40 authored by Christel Devaud, Jennifer Westwood, Liza John, Jacqueline Flynn, Sophie Paquet-Fifield, Connie Duong, Carmen Yong, Hollie Pegram, Steven Stacker, Marc Achen, Trina Stewart, Linda Snyder, Michele Teng, Mark Smyth, Phillip Darcy, Michael Kershaw
The tumor microenvironment can promote tumor growth and reduce treatment efficacy. Tumors can occur in many sites in the body, but how surrounding normal tissues at different anatomical sites affect tumor microenvironments and their subsequent response to therapy is not known.We demonstrated that tumors from renal, colon, or prostate cell lines in orthotopic locations responded to immunotherapy consisting of three agonist antibodies, termed Tri-mAb, to a much lesser extent than the same tumor type located subcutaneously. A tissue-specific response to Tri-mAb was confirmed by ex vivo separation of subcutaneous (SC) or orthotopic tumor cells from stromal cells, followed by reinjection of tumor cells into the opposite site. Compared with SC tumors, orthotopic tumors had a microenvironment associated with a type 2 immune response, related to immunosuppression, and an involvement of alternatively activated macrophages in the kidney model. Orthotopic kidney tumors were more highly vascularized than SC tumors. Neutralizing the macrophage- and Th2-associated molecules chemokine (C-C motif) ligand 2 or interleukin-13 led to a significantly improved therapeutic effect. This study highlights the importance of the tissue of implantation in sculpting the tumor microenvironment. These are important fundamental issues in tumor biology and crucial factors to consider in the design of experimental models and treatment strategies.

History

Journal

Molecular Therapy

Volume

22

Issue

1

Start page

18

End page

27

Total pages

10

Publisher

Nature Publishing Group

Place published

United States

Language

English

Copyright

© The American Society of Gene and Cell Therapy

Former Identifier

2006055094

Esploro creation date

2020-06-22

Fedora creation date

2015-09-29