Interactions between T Cells Responding to Concurrent Mycobacterial and Influenza Infections

Interactions between T Cells Responding to Concurrent Mycobacterial and Influenza Infections

CD4(+) T cells are central in mediating granuloma formation and limiting growth and dissemination of mycobacterial infections. To determine whether T cells responding to influenza infection can interact with T cells responding to Mycobacterium bovis bacille Calmette-Guérin (BCG) infection and disrup...

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Veröffentlicht in:Journal of Immunology 2006-12, Vol.177 (12), p.8456-8465
Hauptverfasser: Co, Dominic O, Hogan, Laura H, Karman, Jozsef, Heninger, Erika, Vang, Shoua, Wells, Krisna, Kawaoka, Yoshihiro, Sandor, Matyas
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Sprache:eng
Schlagworte:
Animals
Antigens - immunology
Cell Communication - immunology
Chickens
Clone Cells
Columbidae
Cytochromes c - immunology
Granuloma - etiology
Granuloma - immunology
Humans
Immunity
Influenza virus
Influenza, Human - immunology
Mice
Mice, Knockout
Muramidase - immunology
Mycobacterium bovis
T-Lymphocytes - immunology
T-Lymphocytes - physiology
Tuberculosis - immunology
Tuberculosis - pathology
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container_end_page 8465
container_issue 12
container_start_page 8456
container_title Journal of Immunology
container_volume 177
creator Co, Dominic O
Hogan, Laura H
Karman, Jozsef
Heninger, Erika
Vang, Shoua
Wells, Krisna
Kawaoka, Yoshihiro
Sandor, Matyas
description CD4(+) T cells are central in mediating granuloma formation and limiting growth and dissemination of mycobacterial infections. To determine whether T cells responding to influenza infection can interact with T cells responding to Mycobacterium bovis bacille Calmette-Guérin (BCG) infection and disrupt granuloma formation, we infected mice containing two monoclonal T cell populations specific for the model Ags pigeon cytochrome c (PCC) and hen egg lysozyme (HEL). These mice were chronically infected with PCC epitope-tagged BCG (PCC-BCG) and acutely infected with HEL epitope-tagged influenza virus (HEL-flu). In these mice, PCC-BCG infection is much more abundant in the liver than the lung, whereas HEL-flu infection is localized to the lung. We observe that both T cells have access to both inflammatory sites, but that PCC-specific T cells dominate the PCC-BCG inflammatory site in the liver, whereas HEL-specific T cells dominate the HEL-flu inflammatory site in the lung. Influenza infection, in the absence of an influenza-specific T cell response, is able to increase the activation state and IFN-gamma secretion of PCC-BCG-specific T cells in the granuloma. Activation of HEL-specific T cells allows them to secrete IFN-gamma and contribute to protection in the granuloma. Ultimately, infection with influenza has little effect on bacterial load, and bacteria do not disseminate. In summary, these data illustrate complex interactions between T cell responses to infectious agents that can affect effector responses to pathogens.
doi_str_mv 10.4049/jimmunol.177.12.8456
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To determine whether T cells responding to influenza infection can interact with T cells responding to Mycobacterium bovis bacille Calmette-Guérin (BCG) infection and disrupt granuloma formation, we infected mice containing two monoclonal T cell populations specific for the model Ags pigeon cytochrome c (PCC) and hen egg lysozyme (HEL). These mice were chronically infected with PCC epitope-tagged BCG (PCC-BCG) and acutely infected with HEL epitope-tagged influenza virus (HEL-flu). In these mice, PCC-BCG infection is much more abundant in the liver than the lung, whereas HEL-flu infection is localized to the lung. We observe that both T cells have access to both inflammatory sites, but that PCC-specific T cells dominate the PCC-BCG inflammatory site in the liver, whereas HEL-specific T cells dominate the HEL-flu inflammatory site in the lung. Influenza infection, in the absence of an influenza-specific T cell response, is able to increase the activation state and IFN-gamma secretion of PCC-BCG-specific T cells in the granuloma. Activation of HEL-specific T cells allows them to secrete IFN-gamma and contribute to protection in the granuloma. Ultimately, infection with influenza has little effect on bacterial load, and bacteria do not disseminate. 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subjects Animals
Antigens - immunology
Cell Communication - immunology
Chickens
Clone Cells
Columbidae
Cytochromes c - immunology
Granuloma - etiology
Granuloma - immunology
Humans
Immunity
Influenza virus
Influenza, Human - immunology
Mice
Mice, Knockout
Muramidase - immunology
Mycobacterium bovis
T-Lymphocytes - immunology
T-Lymphocytes - physiology
Tuberculosis - immunology
Tuberculosis - pathology
title Interactions between T Cells Responding to Concurrent Mycobacterial and Influenza Infections
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