Manning the barricades: lung fibroblasts and CD4+ T cells as the last line of defence against bacterial invasion?
Manning the barricades: lung fibroblasts and CD4+ T cells as the last line of defence against bacterial invasion?
Fibroblasts are a major structural cell in the human lung, being responsible for the production of extracellular matrix components that provide the intricate structure necessary for correct lung function. Generally located in the submucosa, fibroblasts do not usually directly interact with the commensal microbes we now know are resident in the airways. However, during situations where alveolar macrophages and epithelial cells are impaired, for example during severe viral infections leading to pneumonia, bacteria can invade the lung mesenchyme. In these circumstances, fibroblasts may represent another immunological barrier to bacterial invasion, not just as innate immune effectors but also by interacting with migrating and tissue-resident adaptive immune cell populations, such as CD4+ T cells. The cytokines produced by CD4+ T helper cells are integral in directing appropriate innate and adaptive immune responses against bacteria but the nature of fibroblast-CD4+ cell interaction, unlike the CD8+ T cell interaction, is not clearly established. Here, we review the responses of lung fibroblasts to bacteria and discuss emerging data indicating a key role for these cells in directly presenting bacterial antigens to CD4+ T cells.
367-378
Hutton, Andrew J.
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Warner, Jane A.
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Staples, Karl J.
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5 November 2018
Hutton, Andrew J.
1b19a9ff-f942-4e5a-a2ff-62e2c84d2328
Warner, Jane A.
8571b049-31bb-4a2a-a3c7-4184be20fe25
Staples, Karl J.
e0e9d80f-0aed-435f-bd75-0c8818491fee
Hutton, Andrew J., Warner, Jane A. and Staples, Karl J.
(2018)
Manning the barricades: lung fibroblasts and CD4+ T cells as the last line of defence against bacterial invasion?
Critical Reviews in Immunology, 38 (5), .
(doi:10.1615/CritRevImmunol.2018026611).
Abstract
Fibroblasts are a major structural cell in the human lung, being responsible for the production of extracellular matrix components that provide the intricate structure necessary for correct lung function. Generally located in the submucosa, fibroblasts do not usually directly interact with the commensal microbes we now know are resident in the airways. However, during situations where alveolar macrophages and epithelial cells are impaired, for example during severe viral infections leading to pneumonia, bacteria can invade the lung mesenchyme. In these circumstances, fibroblasts may represent another immunological barrier to bacterial invasion, not just as innate immune effectors but also by interacting with migrating and tissue-resident adaptive immune cell populations, such as CD4+ T cells. The cytokines produced by CD4+ T helper cells are integral in directing appropriate innate and adaptive immune responses against bacteria but the nature of fibroblast-CD4+ cell interaction, unlike the CD8+ T cell interaction, is not clearly established. Here, we review the responses of lung fibroblasts to bacteria and discuss emerging data indicating a key role for these cells in directly presenting bacterial antigens to CD4+ T cells.
Text
T cell-fibroblast review 2018-09-17 clean+Fig
- Accepted Manuscript
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Accepted/In Press date: 26 September 2018
Published date: 5 November 2018
Identifiers
Local EPrints ID: 423689
URI: http://eprints.soton.ac.uk/id/eprint/423689
ISSN: 1040-8401
PURE UUID: 529d5072-4da8-4dba-9a8b-9d1eb878a05b
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Date deposited: 27 Sep 2018 16:30
Last modified: 16 Mar 2024 07:07
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Author:
Andrew J. Hutton
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