Tumour-infiltrating lymphocytes bear the 75 kDa tumour necrosis factor receptor

L. Trentin; R. Zambello; P. Bulian; A. Cerutti; C. Enthammer; M. Cassatella; D. Nitti; M. Lise; C. Agostini; C. Semenzato

doi:10.1038/bjc.1995.50

Tumour-infiltrating lymphocytes bear the 75 kDa tumour necrosis factor receptor

L. Trentin, R. Zambello, P. Bulian, A. Cerutti, C. Enthammer, M. Cassatella, D. Nitti, M. Lise, C. Agostini, C. Semenzato

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Abstract

Tumour necrosis factor α (TNF-α) is a cytokine with a variety of immunological properties. The identification of two receptors for this molecule, i.e. the 75 kDa and the 55 kDa TNF receptors (TNF-R), recently clarified the mechanisms through which this cytokine provides its wide range of immunomodulatory activities. In this study we have investigated the expression and the functional properties of these receptors on tumour-infiltrating lymphocytes (TILs) recovered from 17 patients with solid cancers (melanoma, colorectal carcinoma and lung cancer). To this end, TIL lines and freshly isolated TILs were evaluated for (a) the expression and the functional role of TNF receptors following culture in the presence of interleukin 2 (IL-2) and (b) the production of TNF-α following culture with IL-2 and the role of this cytokine in IL-2-driven TIL proliferation. Flow cytometry analysis demonstrated that TILs bear the 75 kDa TNF-R. Moreover, TIL lines express detectable messages for TNF-α and release this cytokine. Functional in vitro studies have shown that anti-TNF-α, as well as anti-75 kDa TNF-R antibodies, are able to inhibit the IL-2-induced TIL proliferation. These data demonstrate that TILs are equipped with a fully functional TNF-R system and suggest a putative role for this receptor and its ligand in the activation and expression of TILs following immunotherapy with IL-2.

Original language	English
Pages (from-to)	240-245
Number of pages	6
Journal	British Journal of Cancer
Volume	71
Issue number	2
DOIs	https://doi.org/10.1038/bjc.1995.50
State	Published - Feb 1995
Externally published	Yes

Keywords

IL-2-driven growth
TNF receptors
Til

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10.1038/bjc.1995.50

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@article{363edcdce9cd476ea924b4cf0cb718a0,

title = "Tumour-infiltrating lymphocytes bear the 75 kDa tumour necrosis factor receptor",

abstract = "Tumour necrosis factor α (TNF-α) is a cytokine with a variety of immunological properties. The identification of two receptors for this molecule, i.e. the 75 kDa and the 55 kDa TNF receptors (TNF-R), recently clarified the mechanisms through which this cytokine provides its wide range of immunomodulatory activities. In this study we have investigated the expression and the functional properties of these receptors on tumour-infiltrating lymphocytes (TILs) recovered from 17 patients with solid cancers (melanoma, colorectal carcinoma and lung cancer). To this end, TIL lines and freshly isolated TILs were evaluated for (a) the expression and the functional role of TNF receptors following culture in the presence of interleukin 2 (IL-2) and (b) the production of TNF-α following culture with IL-2 and the role of this cytokine in IL-2-driven TIL proliferation. Flow cytometry analysis demonstrated that TILs bear the 75 kDa TNF-R. Moreover, TIL lines express detectable messages for TNF-α and release this cytokine. Functional in vitro studies have shown that anti-TNF-α, as well as anti-75 kDa TNF-R antibodies, are able to inhibit the IL-2-induced TIL proliferation. These data demonstrate that TILs are equipped with a fully functional TNF-R system and suggest a putative role for this receptor and its ligand in the activation and expression of TILs following immunotherapy with IL-2.",

keywords = "IL-2-driven growth, TNF receptors, Til",

author = "L. Trentin and R. Zambello and P. Bulian and A. Cerutti and C. Enthammer and M. Cassatella and D. Nitti and M. Lise and C. Agostini and C. Semenzato",

note = "Funding Information: Acknowle es The authors wish to thank Biogen (Cambridge, MA, USA) for supplying recombinant IL-2; Dr M Brockhaus (Bask, Switzerland) for providing utr-I and htr-9 MAbs; Dr G Trinchieri (Philadelphia, PA, USA) for providing B154.9 and B154.7 MAbs; Genentech (San Francisco, CA, USA) for kindly providing TNF-a cDNA; and Mr Martin Donach for his help in the preparation of the manuscript. This study was supported by grants from the Italian Association for Cancer Research (AIRC, Milan), by the National Research Council (CNR, Rome), Project Clinical Applications of Oncological Research and by Progetto Finalizato Regione Veneto. Drs L Tren- tin and R Zambello are recipients of a fellowship from the Ministero della Sanita, Istituto Superiore di Sanita (Rome); Dr P Bulian is a recipient of a fellowship from Associazione Italiana per la Ricerca sul Cancro (AIRC, Milan).",

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doi = "10.1038/bjc.1995.50",

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T1 - Tumour-infiltrating lymphocytes bear the 75 kDa tumour necrosis factor receptor

AU - Trentin, L.

AU - Zambello, R.

AU - Bulian, P.

AU - Cerutti, A.

AU - Enthammer, C.

AU - Cassatella, M.

AU - Nitti, D.

AU - Lise, M.

AU - Agostini, C.

AU - Semenzato, C.

N1 - Funding Information: Acknowle es The authors wish to thank Biogen (Cambridge, MA, USA) for supplying recombinant IL-2; Dr M Brockhaus (Bask, Switzerland) for providing utr-I and htr-9 MAbs; Dr G Trinchieri (Philadelphia, PA, USA) for providing B154.9 and B154.7 MAbs; Genentech (San Francisco, CA, USA) for kindly providing TNF-a cDNA; and Mr Martin Donach for his help in the preparation of the manuscript. This study was supported by grants from the Italian Association for Cancer Research (AIRC, Milan), by the National Research Council (CNR, Rome), Project Clinical Applications of Oncological Research and by Progetto Finalizato Regione Veneto. Drs L Tren- tin and R Zambello are recipients of a fellowship from the Ministero della Sanita, Istituto Superiore di Sanita (Rome); Dr P Bulian is a recipient of a fellowship from Associazione Italiana per la Ricerca sul Cancro (AIRC, Milan).

PY - 1995/2

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N2 - Tumour necrosis factor α (TNF-α) is a cytokine with a variety of immunological properties. The identification of two receptors for this molecule, i.e. the 75 kDa and the 55 kDa TNF receptors (TNF-R), recently clarified the mechanisms through which this cytokine provides its wide range of immunomodulatory activities. In this study we have investigated the expression and the functional properties of these receptors on tumour-infiltrating lymphocytes (TILs) recovered from 17 patients with solid cancers (melanoma, colorectal carcinoma and lung cancer). To this end, TIL lines and freshly isolated TILs were evaluated for (a) the expression and the functional role of TNF receptors following culture in the presence of interleukin 2 (IL-2) and (b) the production of TNF-α following culture with IL-2 and the role of this cytokine in IL-2-driven TIL proliferation. Flow cytometry analysis demonstrated that TILs bear the 75 kDa TNF-R. Moreover, TIL lines express detectable messages for TNF-α and release this cytokine. Functional in vitro studies have shown that anti-TNF-α, as well as anti-75 kDa TNF-R antibodies, are able to inhibit the IL-2-induced TIL proliferation. These data demonstrate that TILs are equipped with a fully functional TNF-R system and suggest a putative role for this receptor and its ligand in the activation and expression of TILs following immunotherapy with IL-2.

AB - Tumour necrosis factor α (TNF-α) is a cytokine with a variety of immunological properties. The identification of two receptors for this molecule, i.e. the 75 kDa and the 55 kDa TNF receptors (TNF-R), recently clarified the mechanisms through which this cytokine provides its wide range of immunomodulatory activities. In this study we have investigated the expression and the functional properties of these receptors on tumour-infiltrating lymphocytes (TILs) recovered from 17 patients with solid cancers (melanoma, colorectal carcinoma and lung cancer). To this end, TIL lines and freshly isolated TILs were evaluated for (a) the expression and the functional role of TNF receptors following culture in the presence of interleukin 2 (IL-2) and (b) the production of TNF-α following culture with IL-2 and the role of this cytokine in IL-2-driven TIL proliferation. Flow cytometry analysis demonstrated that TILs bear the 75 kDa TNF-R. Moreover, TIL lines express detectable messages for TNF-α and release this cytokine. Functional in vitro studies have shown that anti-TNF-α, as well as anti-75 kDa TNF-R antibodies, are able to inhibit the IL-2-induced TIL proliferation. These data demonstrate that TILs are equipped with a fully functional TNF-R system and suggest a putative role for this receptor and its ligand in the activation and expression of TILs following immunotherapy with IL-2.

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Tumour-infiltrating lymphocytes bear the 75 kDa tumour necrosis factor receptor

Abstract

Keywords

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