TGF-β builds a dual immune barrier in colorectal cancer by impairing T cell recruitment and instructing immunosuppressive SPP1+ macrophages.

Ana Henriques; Maria Salvany-Celades; Paula Nieto; Sergio Palomo-Ponce; Marta Sevillano; Xavier Hernando-Momblona; Emily Middendorp-Guerra; Montserrat Llanses Martinez; Elisabeth Marjolein Haak; Juan Nieto; Ginevra Caratú; Domenica Marchese; Max Ruiz Gil; Sebastien Tosi; Theresa Suckert; Jordi Badia-Ramentol; Adrià Caballé-Mestres; Carolina Sanchez-Zarzalejo; Lidia Mateo; Daniele V F Tauriello; Antoni Riera; Elena Sancho; Camille Stephan-Otto Attolini; Alejandro Prados; Holger Heyn; Eduard Batlle

doi:10.1038/s41588-025-02380-2

TGF-β builds a dual immune barrier in colorectal cancer by impairing T cell recruitment and instructing immunosuppressive SPP1⁺ macrophages.

Ana Henriques
, Maria Salvany-Celades
, Paula Nieto
, Sergio Palomo-Ponce
, Marta Sevillano
, Xavier Hernando-Momblona
, Emily Middendorp-Guerra
, Montserrat Llanses Martinez
, Elisabeth Marjolein Haak
, Juan Nieto
, Ginevra Caratú
, Domenica Marchese
, Max Ruiz Gil
, Sebastien Tosi
, Theresa Suckert
, Jordi Badia-Ramentol
, Adrià Caballé-Mestres
, Carolina Sanchez-Zarzalejo
, Lidia Mateo
, Daniele V F Tauriello

Antoni Riera, Elena Sancho, Camille Stephan-Otto Attolini, Alejandro Prados, Holger Heyn, Eduard Batlle

Medical Oncology

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Transforming growth factor β (TGF-β) signaling in the tumor microenvironment predicts resistance to immune checkpoint blockade (ICB). While TGF-β inhibition enhances ICB efficacy in murine cancer models, clinical trials have yet to demonstrate benefit, underscoring the need to better understand its immunoregulatory roles across disease contexts. Using mouse models of advanced colorectal cancer and patient-derived data, we demonstrate that TGF-β impairs antitumor immunity at multiple levels in liver metastases. It acts directly on T cells to block recruitment of peripheral memory CD8 + T cells, thereby limiting the effectiveness of ICB. Concurrently, TGF-β instructs tumor-associated macrophages to suppress clonal expansion of newly arrived T cells by inducing SPP1 expression. This extracellular matrix protein promotes collagen deposition and accumulation of tumor-associated macrophages and fibroblasts, ultimately driving ICB resistance. Our findings reveal how TGF-β coordinates immunosuppressive mechanisms across innate and adaptive immune compartments to promote metastasis, offering new avenues to improve immunotherapy in colorectal cancer.

Original language	English
Number of pages	46
Journal	Nature Genetics
DOIs	https://doi.org/10.1038/s41588-025-02380-2
Publication status	E-pub ahead of print - 7 Nov 2025

Bibliographical note

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This output contributes to the following UN Sustainable Development Goals (SDGs)

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Henriques, A., Salvany-Celades, M., Nieto, P., Palomo-Ponce, S., Sevillano, M., Hernando-Momblona, X., Middendorp-Guerra, E., Llanses Martinez, M., Haak, E. M., Nieto, J., Caratú, G., Marchese, D., Ruiz Gil, M., Tosi, S., Suckert, T., Badia-Ramentol, J., Caballé-Mestres, A., Sanchez-Zarzalejo, C., Mateo, L., ... Batlle, E. (2025). TGF-β builds a dual immune barrier in colorectal cancer by impairing T cell recruitment and instructing immunosuppressive SPP1⁺ macrophages. Nature Genetics. Advance online publication. https://doi.org/10.1038/s41588-025-02380-2

@article{0d80d64e18d744799dc2eee2b6b84ee4,

title = "TGF-β builds a dual immune barrier in colorectal cancer by impairing T cell recruitment and instructing immunosuppressive SPP1+ macrophages.",

abstract = "Transforming growth factor β (TGF-β) signaling in the tumor microenvironment predicts resistance to immune checkpoint blockade (ICB). While TGF-β inhibition enhances ICB efficacy in murine cancer models, clinical trials have yet to demonstrate benefit, underscoring the need to better understand its immunoregulatory roles across disease contexts. Using mouse models of advanced colorectal cancer and patient-derived data, we demonstrate that TGF-β impairs antitumor immunity at multiple levels in liver metastases. It acts directly on T cells to block recruitment of peripheral memory CD8 + T cells, thereby limiting the effectiveness of ICB. Concurrently, TGF-β instructs tumor-associated macrophages to suppress clonal expansion of newly arrived T cells by inducing SPP1 expression. This extracellular matrix protein promotes collagen deposition and accumulation of tumor-associated macrophages and fibroblasts, ultimately driving ICB resistance. Our findings reveal how TGF-β coordinates immunosuppressive mechanisms across innate and adaptive immune compartments to promote metastasis, offering new avenues to improve immunotherapy in colorectal cancer. ",

author = "Ana Henriques and Maria Salvany-Celades and Paula Nieto and Sergio Palomo-Ponce and Marta Sevillano and Xavier Hernando-Momblona and Emily Middendorp-Guerra and \{Llanses Martinez\}, Montserrat and Haak, \{Elisabeth Marjolein\} and Juan Nieto and Ginevra Carat{\'u} and Domenica Marchese and \{Ruiz Gil\}, Max and Sebastien Tosi and Theresa Suckert and Jordi Badia-Ramentol and Adri{\`a} Caball{\'e}-Mestres and Carolina Sanchez-Zarzalejo and Lidia Mateo and Tauriello, \{Daniele V F\} and Antoni Riera and Elena Sancho and Attolini, \{Camille Stephan-Otto\} and Alejandro Prados and Holger Heyn and Eduard Batlle",

note = "{\textcopyright} 2025. The Author(s), under exclusive licence to Springer Nature America, Inc.",

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doi = "10.1038/s41588-025-02380-2",

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Henriques, A, Salvany-Celades, M, Nieto, P, Palomo-Ponce, S, Sevillano, M, Hernando-Momblona, X, Middendorp-Guerra, E, Llanses Martinez, M, Haak, EM, Nieto, J, Caratú, G, Marchese, D, Ruiz Gil, M, Tosi, S, Suckert, T, Badia-Ramentol, J, Caballé-Mestres, A, Sanchez-Zarzalejo, C, Mateo, L, Tauriello, DVF, Riera, A, Sancho, E, Attolini, CS-O, Prados, A, Heyn, H & Batlle, E 2025, 'TGF-β builds a dual immune barrier in colorectal cancer by impairing T cell recruitment and instructing immunosuppressive SPP1⁺ macrophages.', Nature Genetics. https://doi.org/10.1038/s41588-025-02380-2

TY - JOUR

T1 - TGF-β builds a dual immune barrier in colorectal cancer by impairing T cell recruitment and instructing immunosuppressive SPP1+ macrophages.

AU - Henriques, Ana

AU - Salvany-Celades, Maria

AU - Nieto, Paula

AU - Palomo-Ponce, Sergio

AU - Sevillano, Marta

AU - Hernando-Momblona, Xavier

AU - Middendorp-Guerra, Emily

AU - Llanses Martinez, Montserrat

AU - Haak, Elisabeth Marjolein

AU - Nieto, Juan

AU - Caratú, Ginevra

AU - Marchese, Domenica

AU - Ruiz Gil, Max

AU - Tosi, Sebastien

AU - Suckert, Theresa

AU - Badia-Ramentol, Jordi

AU - Caballé-Mestres, Adrià

AU - Sanchez-Zarzalejo, Carolina

AU - Mateo, Lidia

AU - Tauriello, Daniele V F

AU - Riera, Antoni

AU - Sancho, Elena

AU - Attolini, Camille Stephan-Otto

AU - Prados, Alejandro

AU - Heyn, Holger

AU - Batlle, Eduard

PY - 2025/11/7

Y1 - 2025/11/7

N2 - Transforming growth factor β (TGF-β) signaling in the tumor microenvironment predicts resistance to immune checkpoint blockade (ICB). While TGF-β inhibition enhances ICB efficacy in murine cancer models, clinical trials have yet to demonstrate benefit, underscoring the need to better understand its immunoregulatory roles across disease contexts. Using mouse models of advanced colorectal cancer and patient-derived data, we demonstrate that TGF-β impairs antitumor immunity at multiple levels in liver metastases. It acts directly on T cells to block recruitment of peripheral memory CD8 + T cells, thereby limiting the effectiveness of ICB. Concurrently, TGF-β instructs tumor-associated macrophages to suppress clonal expansion of newly arrived T cells by inducing SPP1 expression. This extracellular matrix protein promotes collagen deposition and accumulation of tumor-associated macrophages and fibroblasts, ultimately driving ICB resistance. Our findings reveal how TGF-β coordinates immunosuppressive mechanisms across innate and adaptive immune compartments to promote metastasis, offering new avenues to improve immunotherapy in colorectal cancer.

AB - Transforming growth factor β (TGF-β) signaling in the tumor microenvironment predicts resistance to immune checkpoint blockade (ICB). While TGF-β inhibition enhances ICB efficacy in murine cancer models, clinical trials have yet to demonstrate benefit, underscoring the need to better understand its immunoregulatory roles across disease contexts. Using mouse models of advanced colorectal cancer and patient-derived data, we demonstrate that TGF-β impairs antitumor immunity at multiple levels in liver metastases. It acts directly on T cells to block recruitment of peripheral memory CD8 + T cells, thereby limiting the effectiveness of ICB. Concurrently, TGF-β instructs tumor-associated macrophages to suppress clonal expansion of newly arrived T cells by inducing SPP1 expression. This extracellular matrix protein promotes collagen deposition and accumulation of tumor-associated macrophages and fibroblasts, ultimately driving ICB resistance. Our findings reveal how TGF-β coordinates immunosuppressive mechanisms across innate and adaptive immune compartments to promote metastasis, offering new avenues to improve immunotherapy in colorectal cancer.

UR - https://www.scopus.com/pages/publications/105021243705

U2 - 10.1038/s41588-025-02380-2

DO - 10.1038/s41588-025-02380-2

M3 - Article

C2 - 41203813

SN - 1061-4036

JO - Nature Genetics

JF - Nature Genetics

ER -

TGF-β builds a dual immune barrier in colorectal cancer by impairing T cell recruitment and instructing immunosuppressive SPP1⁺ macrophages.

Abstract

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