Characterisation of leukocytes in a human skin blister model of acute inflammation and resolution.
Characterisation of leukocytes in a human skin blister model of acute inflammation and resolution.
There is an increasing need to understand the leukocytes and soluble mediators that drive acute inflammation and bring about its resolution in humans. We therefore carried out an extensive characterisation of the cantharidin skin blister model in healthy male volunteers. A novel fluorescence staining protocol was designed and implemented, which facilitated the identification of cell populations by flow cytometry. We observed that at the onset phase, 24 h after blister formation, the predominant cells were CD16hi/CD66b+ PMNs followed by HLA-DR+/CD14+ monocytes/macrophages, CD11c+ and CD141+ dendritic cells as well as Siglec-8+ eosinophils. CD3+ T cells, CD19+ B cells and CD56+ NK cells were also present, but in comparatively fewer numbers. During resolution, 72 h following blister induction, numbers of PMNs declined whilst the numbers of monocyte/macrophages remain unchanged, though they upregulated expression of CD16 and CD163. In contrast, the overall numbers of dendritic cells and Siglec-8+ eosinophils increased. Post hoc analysis of these data revealed that of the inflammatory cytokines measured, TNF-α but not IL-1β or IL-8 correlated with increased PMN numbers at the onset. Volunteers with the greatest PMN infiltration at onset displayed the fastest clearance rates for these cells at resolution. Collectively, these data provide insight into the cells that occupy acute resolving blister in humans, the soluble mediators that may control their influx as well as the phenotype of mononuclear phagocytes that predominate the resolution phase. Further use of this model will improve our understanding of the evolution and resolution of inflammation in humans, how defects in these over-lapping pathways may contribute to the variability in disease longevity/chronicity, and lends itself to the screen of putative anti-inflammatory or pro-resolution therapies.
Jenner, William
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Motwani, M
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Veighey, K
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Newson, J
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Audzevich, T
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Nicolaou, A
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Murphy, S
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Macallister, R
9f4b26b2-72e1-4ccf-9338-362d6193085b
Gilroy, DW
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6 March 2014
Jenner, William
87440735-1775-4334-84cf-e7426a6a7fed
Motwani, M
d791ea3e-2e47-4a56-b6b1-61034852fbe8
Veighey, K
2adbaf5c-141a-44bd-a7eb-faf14e0ca251
Newson, J
8aea0732-0509-4432-9b9e-b3c8b2ef3301
Audzevich, T
d878aa95-a797-44d6-a000-56e123b48697
Nicolaou, A
6f2cbaf9-65a1-4152-867f-0d0e7d604a65
Murphy, S
28dd5096-c819-44c7-b85c-2eafdef9042b
Macallister, R
9f4b26b2-72e1-4ccf-9338-362d6193085b
Gilroy, DW
98a3fa29-4c31-46a5-9f19-2fffd59db792
Jenner, William, Motwani, M, Veighey, K, Newson, J, Audzevich, T, Nicolaou, A, Murphy, S, Macallister, R and Gilroy, DW
(2014)
Characterisation of leukocytes in a human skin blister model of acute inflammation and resolution.
PLoS ONE.
(doi:10.1371/journal.pone.0089375).
Abstract
There is an increasing need to understand the leukocytes and soluble mediators that drive acute inflammation and bring about its resolution in humans. We therefore carried out an extensive characterisation of the cantharidin skin blister model in healthy male volunteers. A novel fluorescence staining protocol was designed and implemented, which facilitated the identification of cell populations by flow cytometry. We observed that at the onset phase, 24 h after blister formation, the predominant cells were CD16hi/CD66b+ PMNs followed by HLA-DR+/CD14+ monocytes/macrophages, CD11c+ and CD141+ dendritic cells as well as Siglec-8+ eosinophils. CD3+ T cells, CD19+ B cells and CD56+ NK cells were also present, but in comparatively fewer numbers. During resolution, 72 h following blister induction, numbers of PMNs declined whilst the numbers of monocyte/macrophages remain unchanged, though they upregulated expression of CD16 and CD163. In contrast, the overall numbers of dendritic cells and Siglec-8+ eosinophils increased. Post hoc analysis of these data revealed that of the inflammatory cytokines measured, TNF-α but not IL-1β or IL-8 correlated with increased PMN numbers at the onset. Volunteers with the greatest PMN infiltration at onset displayed the fastest clearance rates for these cells at resolution. Collectively, these data provide insight into the cells that occupy acute resolving blister in humans, the soluble mediators that may control their influx as well as the phenotype of mononuclear phagocytes that predominate the resolution phase. Further use of this model will improve our understanding of the evolution and resolution of inflammation in humans, how defects in these over-lapping pathways may contribute to the variability in disease longevity/chronicity, and lends itself to the screen of putative anti-inflammatory or pro-resolution therapies.
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Accepted/In Press date: 18 January 2014
Published date: 6 March 2014
Identifiers
Local EPrints ID: 495057
URI: http://eprints.soton.ac.uk/id/eprint/495057
ISSN: 1932-6203
PURE UUID: eb01544e-ef83-4a87-b4e2-cc3f4dc75d67
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Date deposited: 28 Oct 2024 17:54
Last modified: 29 Oct 2024 02:57
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Author:
William Jenner
Author:
M Motwani
Author:
J Newson
Author:
T Audzevich
Author:
A Nicolaou
Author:
S Murphy
Author:
R Macallister
Author:
DW Gilroy
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