Marketing deregulated expression of anti-apoptotic proteins belonging to the Bcl-2 family in neutrophils as a potential therapy against periodontal disease. In vitro and in vivo analysis. (Q84300): Difference between revisions

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description / endescription / en
Project in Poland financed by DG Regio
Project Q84300 in Poland
description / pldescription / pl
Projekt w Polsce finansowany przez DG Regio
Projekt Q84300 w Polsce

Revision as of 05:23, 29 October 2020

Project Q84300 in Poland
Language Label Description Also known as
English
Marketing deregulated expression of anti-apoptotic proteins belonging to the Bcl-2 family in neutrophils as a potential therapy against periodontal disease. In vitro and in vivo analysis.
Project Q84300 in Poland

    Statements

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    2,000,000.0 zloty
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    480,000.0 Euro
    13 January 2020
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    2,000,000.0 zloty
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    480,000.0 Euro
    13 January 2020
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    100.0 percent
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    1 April 2019
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    31 March 2022
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    UNIWERSYTET JAGIELLOŃSKI
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    Chronic periodontal disease(PD) is one of the most frequent inflammatory diseases affecting 11.2% of the world’s population and representing a prominent public health burden. Risk factors for developing PD are cigarette smoking, diabetes, osteoporosis, and infections with periodontal pathogens(i.e. Porphyromonas gingivalis). The pathogenesis of PD is associated with an over-reactive host inflammatory response to P.gingivalis. Current literature implicates hyper-reactive neutrophils as the main immune cell type responsible for the tissue damage and the disease progression. Neutrophils have very short lifespan, controlled by the Bcl-2 family proteins, but it can be significantly prolonged during the infection. Therefore, I hypothesize that hyper-activity and prolonged survival of neutrophils induced by P.gingivalis through the increased expression of pro-survival members of the Bcl-2 family proteins is a novel, yet uncharacterized mechanism strongly contributing to the development of PD. (Polish)
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    Chronic periodontal disease(PD) is one of the most frequent inflammatory diseases affecting 11.2 % of the world’s population and representing a prominent public health burden. Risk factors for developing PD are cigarette smoking, diabetes, osteoporosis, and infections with periodontal Pathogens(i.e. Porphyromonas gingivalis). The pathogenesis of PD is associated with an over-reactive host inflammatory response to P.gingivalis. Current literature implicates hyper-reactive neutrophils as the main immune cell type responsible for the tissue damage and the disease progression. Neutrophils have very short LifeSpan, controlled by the Bcl-2 family proteins, but it can be significantly prolonged during the infection. Thus, I hypothesise that hyper-activity and prolonged survival of neutrophils induced by P.gingivalis through the increased expression of pro-survival members of the Bcl-2 family proteins is a novel, yet uncharacterised mechanism strongly contributing to the development of PD. (English)
    14 October 2020
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    Identifiers

    POIR.04.04.00-00-42FE/17
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