Modification of signaling pathways of canine Th17 lymphocytes subset to improve Adoptive cellular immunotherapy for humans (Q84267)

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Project Q84267 in Poland
Language Label Description Also known as
English
Modification of signaling pathways of canine Th17 lymphocytes subset to improve Adoptive cellular immunotherapy for humans
Project Q84267 in Poland

    Statements

    country
    Poland
    0 references
    EU contribution
    1,999,750.0 zloty
    0 references
    479,940.0 Euro
    exchange rate to Euro
    0.24 Euro
    point in time
    13 January 2020
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    budget
    1,999,750.0 zloty
    0 references
    479,940.0 Euro
    exchange rate to Euro
    0.24 Euro
    point in time
    13 January 2020
    0 references
    co-financing rate
    100.0 percent
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    start time
    1 November 2017
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    end time
    31 October 2020
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    beneficiary name (string)
    SZKOŁA GŁÓWNA GOSPODARSTWA WIEJSKIEGO W WARSZAWIE
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    summary
    Adoptive cell transfer (ACT) immunotherapy is considered the most promising treatment of cancer; however it is still limited by the use of short-lived and exhausted T cells. Recently, IL-17 producing CD4+ T lymphocytes (Th17 cells) have been shown to be superior in eradication of melanoma in mouse compared to Th1 cells. We propose to determine the expanding ex vivo protocol of Th17 cells from domestic dog in order to support comparative oncology research and improve the ACT-based immunotherapy for humans. We hypothesized that pharmacological manipulation of signaling pathways of canine Th17 cells will enhance their antitumor activity and increase the efficacy of tumor immunotherapy. We plan to evaluate the results on the tumor infiltrating lymphocytes from melanoma-bearing dogs (patients of Veterinary Clinic). The outcomes of the project will provide the rationale for designing next-generation clinical trials for human cancer patients and facilitate development of cell-based drugs. (Polish)
    0 references
    Adoptive cell transfer (ACT) immunotherapy is considered the most promising treatment of cancer; however it is still limited by the use of short-lived and exhausted T cells. Recently, IL-17 producing CD4+ T lymphocytes (Th17 cells) have been shown to be superior in eradication of melanoma in mouse compared to Th1 cells. We propose to determine the expanding ex vivo protocol of Th17 cells from domestic dog in order to support comparative oncology research and improve the ACT-based immunotherapy for humans. We hypothesised that pharmacological manipulation of signaling pathways of canine Th17 cells will enhance their antitumor activity and increase the efficacy of tumor immunotherapy. We plan to evaluate the results on the tumor infiltrating lymphocytes from melanoma-bearing dogs (patients of Veterinary Clinic). The outcomes of the project will provide the rationale for designing next-generation clinical trials for human cancer patients and facilitate development of cell-based drugs. (English)
    point in time
    14 October 2020
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    Identifiers

    Polish Kohesio ID
    POIR.04.04.00-00-3EE9/17
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