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TNF-alpha is critical for antitumor but not antiviral T cell immunity in mice.

TNF-alpha is critical for antitumor but not antiviral T cell immunity in mice. Research Abstract Details 

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  • TNF-alpha is critical for antitumor but not antiviral T cell immunity in mice. Abstract Text:

    thomas calzasciaThomas Calzascia,marc pellegriniMarc Pellegrini, hall Hall,laurent sabbaghLaurent Sabbagh,nobuyuki onoNobuyuki Ono,alisha r elfordAlisha R Elford,tak w makTak W Mak,pamela s ohashiPamela S Ohashi,thomas calzasciaThomas Calzascia,marc pellegriniMarc Pellegrini, hall Hall,laurent sabbaghLaurent Sabbagh,nobuyuki onoNobuyuki Ono,alisha r elfordAlisha R Elford,tak w makTak W Mak,pamela s ohashiPamela S Ohashi,thomas calzasciaThomas Calzascia,marc pellegriniMarc Pellegrini,håkan hallHåkan Hall,laurent sabbaghLaurent Sabbagh,nobuyuki onoNobuyuki Ono,alisha r elfordAlisha R Elford,tak w makTak W Mak,pamela s ohashiPamela S Ohashi,

    TNF-alpha antagonists are widely used in the treatment of inflammatory and autoimmune diseases, but their use is associated with reactivation of latent infections. This highlights the importance of TNF-alpha in immunity to certain pathogens and raises concerns that critical aspects of immune function are impaired in its absence. Unfortunately, the role of TNF-alpha in the regulation of T cell responses is clouded by a myriad of contradictory reports. Here, we show a role for TNF-alpha and its receptors, TNFR1 and TNFR2, specifically in antitumor immunity. TNF-alpha-deficient mice exhibited normal antiviral responses associated with strong inflammation. However, TNF-alpha/TNFR1-mediated signals on APCs and TNF-alpha/TNFR2 signals on T cells were critically required for effective priming, proliferation, and recruitment of tumor-specific T cells. Furthermore, in the absence of TNF-alpha signaling, tumor immune surveillance was severely abrogated. Finally, treatment with a CD40 agonist alone or in combination with TLR2 stimuli was able to rescue proliferation of TNF-alpha-deficient T cells. Therefore, TNF-alpha signaling may be required only for immune responses in conditions of limited immunostimulatory capacity, such as tumor surveillance. Importantly, these results suggest that prolonged continuous TNF-alpha blockade in patients may have long-term complications, including potential tumor development or progression.

    TNF-alpha is critical for antitumor but not antiviral T cell immunity in mice. Publishing Authors By Initials

    t calzasciaT Calzascia,m pellegriniM Pellegrini,h hallH Hall,l sabbaghL Sabbagh,n onoN Ono,ar elfordAR Elford,tw makTW Mak,ps ohashiPS Ohashi,t calzasciaT Calzascia,m pellegriniM Pellegrini,h hallH Hall,l sabbaghL Sabbagh,n onoN Ono,ar elfordAR Elford,tw makTW Mak,ps ohashiPS Ohashi,t calzasciaT Calzascia,m pellegriniM Pellegrini,h hallH Hall,l sabbaghL Sabbagh,n onoN Ono,ar elfordAR Elford,tw makTW Mak,ps ohashiPS Ohashi,

    For similar abstracts research abstracts see: abstracts research

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    TNF-alpha is critical for antitumor but not antiviral T cell immunity in mice. Journal Published:

    PUBLICATION TYPE: Research Support, Non-U.S. Gov

    Journal: The Journal of clinical investigation

    VOLUME: 117

    Page Numbers: 3833-45

    Journal Abbreviation: J. Clin. Invest.

    ISSN: 0021-9738

    DAY: 6

    MONTH: Dec

    YEAR: 2007

    TNF-alpha is critical for antitumor but not antiviral T cell immunity in mice. Information

    Number of References:

    LANGUAGE: eng

    NlmUniqueID: 7802877

    TNF-alpha is critical for antitumor but not antiviral T cell immunity in mice. Keywords Mesh Terms:

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    Grant and Affiliation Information for TNF-alpha is critical for antitumor but not antiviral T cell immunity in mice.

    AFFILIATION: The Campbell Family Institute for Breast Cancer Research, Ontario Cancer Institute, Toronto, Ontario, Canada.

    Country: United States

    United States Research PublicationUnited States Research Publication

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    MEDLINETA: J Clin Invest

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