Humanized Mouse Model of Skin Inflammation Is Characterized by Disturbed Keratinocyte Differentiation and Influx of IL-17A Producing T Cells

Humanized mouse models offer a challenging possibility to study human cell function in vivo. In the huPBL-SCID-huSkin allograft model human skin is transplanted onto immunodeficient mice and allowed to heal. Thereafter allogeneic human peripheral blood mononuclear cells are infused intra peritoneall...

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Autores principales: de Oliveira, Vivian L., Keijsers, Romy R. M. C., van de Kerkhof, Peter C. M., Seyger, Marieke M. B., Fasse, Esther, Svensson, Lars, Latta, Markus, Norsgaard, Hanne, Labuda, Tord, Hupkens, Pieter, van Erp, Piet E. J., Joosten, Irma, Koenen, Hans J. P. M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3477148/
https://www.ncbi.nlm.nih.gov/pubmed/23094018
http://dx.doi.org/10.1371/journal.pone.0045509
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author de Oliveira, Vivian L.
Keijsers, Romy R. M. C.
van de Kerkhof, Peter C. M.
Seyger, Marieke M. B.
Fasse, Esther
Svensson, Lars
Latta, Markus
Norsgaard, Hanne
Labuda, Tord
Hupkens, Pieter
van Erp, Piet E. J.
Joosten, Irma
Koenen, Hans J. P. M.
author_facet de Oliveira, Vivian L.
Keijsers, Romy R. M. C.
van de Kerkhof, Peter C. M.
Seyger, Marieke M. B.
Fasse, Esther
Svensson, Lars
Latta, Markus
Norsgaard, Hanne
Labuda, Tord
Hupkens, Pieter
van Erp, Piet E. J.
Joosten, Irma
Koenen, Hans J. P. M.
author_sort de Oliveira, Vivian L.
collection PubMed
description Humanized mouse models offer a challenging possibility to study human cell function in vivo. In the huPBL-SCID-huSkin allograft model human skin is transplanted onto immunodeficient mice and allowed to heal. Thereafter allogeneic human peripheral blood mononuclear cells are infused intra peritoneally to induce T cell mediated inflammation and microvessel destruction of the human skin. This model has great potential for in vivo study of human immune cells in (skin) inflammatory processes and for preclinical screening of systemically administered immunomodulating agents. Here we studied the inflammatory skin response of human keratinocytes and human T cells and the concomitant systemic human T cell response. As new findings in the inflamed human skin of the huPBL-SCID-huSkin model we here identified: 1. Parameters of dermal pathology that enable precise quantification of the local skin inflammatory response exemplified by acanthosis, increased expression of human β-defensin-2, Elafin, K16, Ki67 and reduced expression of K10 by microscopy and immunohistochemistry. 2. Induction of human cytokines and chemokines using quantitative real-time PCR. 3. Influx of inflammation associated IL-17A-producing human CD4+ and CD8+ T cells as well as immunoregulatory CD4+Foxp3+ cells using immunohistochemistry and -fluorescence, suggesting that active immune regulation is taking place locally in the inflamed skin. 4. Systemic responses that revealed activated and proliferating human CD4+ and CD8+ T cells that acquired homing marker expression of CD62L and CLA. Finally, we demonstrated the value of the newly identified parameters by showing significant changes upon systemic treatment with the T cell inhibitory agents cyclosporine-A and rapamycin. In summary, here we equipped the huPBL-SCID-huSkin humanized mouse model with relevant tools not only to quantify the inflammatory dermal response, but also to monitor the peripheral immune status. This combined approach will gain our understanding of the dermal immunopathology in humans and benefit the development of novel therapeutics for controlling inflammatory skin diseases.
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spelling pubmed-34771482012-10-23 Humanized Mouse Model of Skin Inflammation Is Characterized by Disturbed Keratinocyte Differentiation and Influx of IL-17A Producing T Cells de Oliveira, Vivian L. Keijsers, Romy R. M. C. van de Kerkhof, Peter C. M. Seyger, Marieke M. B. Fasse, Esther Svensson, Lars Latta, Markus Norsgaard, Hanne Labuda, Tord Hupkens, Pieter van Erp, Piet E. J. Joosten, Irma Koenen, Hans J. P. M. PLoS One Research Article Humanized mouse models offer a challenging possibility to study human cell function in vivo. In the huPBL-SCID-huSkin allograft model human skin is transplanted onto immunodeficient mice and allowed to heal. Thereafter allogeneic human peripheral blood mononuclear cells are infused intra peritoneally to induce T cell mediated inflammation and microvessel destruction of the human skin. This model has great potential for in vivo study of human immune cells in (skin) inflammatory processes and for preclinical screening of systemically administered immunomodulating agents. Here we studied the inflammatory skin response of human keratinocytes and human T cells and the concomitant systemic human T cell response. As new findings in the inflamed human skin of the huPBL-SCID-huSkin model we here identified: 1. Parameters of dermal pathology that enable precise quantification of the local skin inflammatory response exemplified by acanthosis, increased expression of human β-defensin-2, Elafin, K16, Ki67 and reduced expression of K10 by microscopy and immunohistochemistry. 2. Induction of human cytokines and chemokines using quantitative real-time PCR. 3. Influx of inflammation associated IL-17A-producing human CD4+ and CD8+ T cells as well as immunoregulatory CD4+Foxp3+ cells using immunohistochemistry and -fluorescence, suggesting that active immune regulation is taking place locally in the inflamed skin. 4. Systemic responses that revealed activated and proliferating human CD4+ and CD8+ T cells that acquired homing marker expression of CD62L and CLA. Finally, we demonstrated the value of the newly identified parameters by showing significant changes upon systemic treatment with the T cell inhibitory agents cyclosporine-A and rapamycin. In summary, here we equipped the huPBL-SCID-huSkin humanized mouse model with relevant tools not only to quantify the inflammatory dermal response, but also to monitor the peripheral immune status. This combined approach will gain our understanding of the dermal immunopathology in humans and benefit the development of novel therapeutics for controlling inflammatory skin diseases. Public Library of Science 2012-10-19 /pmc/articles/PMC3477148/ /pubmed/23094018 http://dx.doi.org/10.1371/journal.pone.0045509 Text en © 2012 de Oliveira et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
de Oliveira, Vivian L.
Keijsers, Romy R. M. C.
van de Kerkhof, Peter C. M.
Seyger, Marieke M. B.
Fasse, Esther
Svensson, Lars
Latta, Markus
Norsgaard, Hanne
Labuda, Tord
Hupkens, Pieter
van Erp, Piet E. J.
Joosten, Irma
Koenen, Hans J. P. M.
Humanized Mouse Model of Skin Inflammation Is Characterized by Disturbed Keratinocyte Differentiation and Influx of IL-17A Producing T Cells
title Humanized Mouse Model of Skin Inflammation Is Characterized by Disturbed Keratinocyte Differentiation and Influx of IL-17A Producing T Cells
title_full Humanized Mouse Model of Skin Inflammation Is Characterized by Disturbed Keratinocyte Differentiation and Influx of IL-17A Producing T Cells
title_fullStr Humanized Mouse Model of Skin Inflammation Is Characterized by Disturbed Keratinocyte Differentiation and Influx of IL-17A Producing T Cells
title_full_unstemmed Humanized Mouse Model of Skin Inflammation Is Characterized by Disturbed Keratinocyte Differentiation and Influx of IL-17A Producing T Cells
title_short Humanized Mouse Model of Skin Inflammation Is Characterized by Disturbed Keratinocyte Differentiation and Influx of IL-17A Producing T Cells
title_sort humanized mouse model of skin inflammation is characterized by disturbed keratinocyte differentiation and influx of il-17a producing t cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3477148/
https://www.ncbi.nlm.nih.gov/pubmed/23094018
http://dx.doi.org/10.1371/journal.pone.0045509
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