The inhibition of TNF-α anti-tumoral properties by blocking antibodies promotes tumor growth in a rat model

Nicolas Larmonier; Dominique Cathelin; Claire Larmonier; Alexandra Nicolas; Delphine Merino; Nona Janikashvili; Sylvain Audia; Andrew Bateman; Jill Thompson; Tim Kottke; Thomas Hartung; Emmanuel Katsanis; Richard Vile; Bernard Bonnotte

doi:10.1016/j.yexcr.2007.03.027

The inhibition of TNF-α anti-tumoral properties by blocking antibodies promotes tumor growth in a rat model

Nicolas Larmonier, Dominique Cathelin, Claire Larmonier, Alexandra Nicolas, Delphine Merino, Nona Janikashvili, Sylvain Audia, Andrew Bateman, Jill Thompson, Tim Kottke, Thomas Hartung, Emmanuel Katsanis, Richard Vile, Bernard Bonnotte

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

29 Scopus citations

Abstract

Tumor necrosis factor (TNF) antagonists represent a milestone in the therapy of autoimmune conditions. Anti-TNF antibodies have been approved for clinical use and during the last eight years thousands of patients have been treated. However, the long-term sequelae of anti-TNF agents in promoting carcinogenesis remain unclear. This study sought to define the role of intra-tumor TNF-α production on cancer cell progression and to determine whether TNF-α antibodies can suppress anti-tumoral immunity. Using an experimental animal tumor model we demonstrate that anti-TNF-α antibodies hinder anti-tumor immune responses and promote growth of immunogenic rat colon tumors (REG) that are always rejected by immunocompetent untreated rats. The major role of TNF-α in the anti-tumoral immune response was confirmed by transfecting progressive and tolerogenic rat colon tumor cells (PRO) with the TNF-α gene. PRO tumor cells secreting TNF-α induce tumor-infiltrating dendritic cell (DC) activation. This triggers a potent immune response leading to tumor rejection and long-lasting immunity. Therefore, the prominent role of TNF-α in anti-tumoral immune responses underscores the need for caution and close surveillance following the administration of TNF inhibitors.

Original language	English (US)
Pages (from-to)	2345-2355
Number of pages	11
Journal	Experimental cell research
Volume	313
Issue number	11
DOIs	https://doi.org/10.1016/j.yexcr.2007.03.027
State	Published - Jul 1 2007
Externally published	Yes

Keywords

Dendritic cells
Gene expression
TNF-α
Tumor immunity

ASJC Scopus subject areas

Cell Biology

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10.1016/j.yexcr.2007.03.027

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Larmonier, N., Cathelin, D., Larmonier, C., Nicolas, A., Merino, D., Janikashvili, N., Audia, S., Bateman, A., Thompson, J., Kottke, T., Hartung, T., Katsanis, E., Vile, R., & Bonnotte, B. (2007). The inhibition of TNF-α anti-tumoral properties by blocking antibodies promotes tumor growth in a rat model. Experimental cell research, 313(11), 2345-2355. https://doi.org/10.1016/j.yexcr.2007.03.027

Larmonier, N, Cathelin, D, Larmonier, C, Nicolas, A, Merino, D, Janikashvili, N, Audia, S, Bateman, A, Thompson, J, Kottke, T, Hartung, T, Katsanis, E, Vile, R & Bonnotte, B 2007, 'The inhibition of TNF-α anti-tumoral properties by blocking antibodies promotes tumor growth in a rat model', Experimental cell research, vol. 313, no. 11, pp. 2345-2355. https://doi.org/10.1016/j.yexcr.2007.03.027

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title = "The inhibition of TNF-α anti-tumoral properties by blocking antibodies promotes tumor growth in a rat model",

abstract = "Tumor necrosis factor (TNF) antagonists represent a milestone in the therapy of autoimmune conditions. Anti-TNF antibodies have been approved for clinical use and during the last eight years thousands of patients have been treated. However, the long-term sequelae of anti-TNF agents in promoting carcinogenesis remain unclear. This study sought to define the role of intra-tumor TNF-α production on cancer cell progression and to determine whether TNF-α antibodies can suppress anti-tumoral immunity. Using an experimental animal tumor model we demonstrate that anti-TNF-α antibodies hinder anti-tumor immune responses and promote growth of immunogenic rat colon tumors (REG) that are always rejected by immunocompetent untreated rats. The major role of TNF-α in the anti-tumoral immune response was confirmed by transfecting progressive and tolerogenic rat colon tumor cells (PRO) with the TNF-α gene. PRO tumor cells secreting TNF-α induce tumor-infiltrating dendritic cell (DC) activation. This triggers a potent immune response leading to tumor rejection and long-lasting immunity. Therefore, the prominent role of TNF-α in anti-tumoral immune responses underscores the need for caution and close surveillance following the administration of TNF inhibitors.",

keywords = "Dendritic cells, Gene expression, TNF-α, Tumor immunity",

author = "Nicolas Larmonier and Dominique Cathelin and Claire Larmonier and Alexandra Nicolas and Delphine Merino and Nona Janikashvili and Sylvain Audia and Andrew Bateman and Jill Thompson and Tim Kottke and Thomas Hartung and Emmanuel Katsanis and Richard Vile and Bernard Bonnotte",

note = "Funding Information: We thank A. Fromentin and E. Situ for excellent technical assistance. This work was supported in part by the Mayo Foundation, the French National League against Cancer (Burgundy and Nievre committees), the Tee Up for Tots and Raise a Racquet for kids Funds. D.C. received funding from the Sa{\^o}ne et Loire League against Cancer. ",

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AU - Larmonier, Nicolas

AU - Cathelin, Dominique

AU - Larmonier, Claire

AU - Nicolas, Alexandra

AU - Merino, Delphine

AU - Janikashvili, Nona

AU - Audia, Sylvain

AU - Bateman, Andrew

AU - Thompson, Jill

AU - Kottke, Tim

AU - Hartung, Thomas

AU - Katsanis, Emmanuel

AU - Vile, Richard

AU - Bonnotte, Bernard

N1 - Funding Information: We thank A. Fromentin and E. Situ for excellent technical assistance. This work was supported in part by the Mayo Foundation, the French National League against Cancer (Burgundy and Nievre committees), the Tee Up for Tots and Raise a Racquet for kids Funds. D.C. received funding from the Saône et Loire League against Cancer.

PY - 2007/7/1

Y1 - 2007/7/1

N2 - Tumor necrosis factor (TNF) antagonists represent a milestone in the therapy of autoimmune conditions. Anti-TNF antibodies have been approved for clinical use and during the last eight years thousands of patients have been treated. However, the long-term sequelae of anti-TNF agents in promoting carcinogenesis remain unclear. This study sought to define the role of intra-tumor TNF-α production on cancer cell progression and to determine whether TNF-α antibodies can suppress anti-tumoral immunity. Using an experimental animal tumor model we demonstrate that anti-TNF-α antibodies hinder anti-tumor immune responses and promote growth of immunogenic rat colon tumors (REG) that are always rejected by immunocompetent untreated rats. The major role of TNF-α in the anti-tumoral immune response was confirmed by transfecting progressive and tolerogenic rat colon tumor cells (PRO) with the TNF-α gene. PRO tumor cells secreting TNF-α induce tumor-infiltrating dendritic cell (DC) activation. This triggers a potent immune response leading to tumor rejection and long-lasting immunity. Therefore, the prominent role of TNF-α in anti-tumoral immune responses underscores the need for caution and close surveillance following the administration of TNF inhibitors.

AB - Tumor necrosis factor (TNF) antagonists represent a milestone in the therapy of autoimmune conditions. Anti-TNF antibodies have been approved for clinical use and during the last eight years thousands of patients have been treated. However, the long-term sequelae of anti-TNF agents in promoting carcinogenesis remain unclear. This study sought to define the role of intra-tumor TNF-α production on cancer cell progression and to determine whether TNF-α antibodies can suppress anti-tumoral immunity. Using an experimental animal tumor model we demonstrate that anti-TNF-α antibodies hinder anti-tumor immune responses and promote growth of immunogenic rat colon tumors (REG) that are always rejected by immunocompetent untreated rats. The major role of TNF-α in the anti-tumoral immune response was confirmed by transfecting progressive and tolerogenic rat colon tumor cells (PRO) with the TNF-α gene. PRO tumor cells secreting TNF-α induce tumor-infiltrating dendritic cell (DC) activation. This triggers a potent immune response leading to tumor rejection and long-lasting immunity. Therefore, the prominent role of TNF-α in anti-tumoral immune responses underscores the need for caution and close surveillance following the administration of TNF inhibitors.

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The inhibition of TNF-α anti-tumoral properties by blocking antibodies promotes tumor growth in a rat model

Abstract

Keywords

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