Acute Liver Injury Is Independent of B Cells or Immunoglobulin M

BACKGROUND & AIMS: Acute liver injury is a clinically important pathology and results in the release of Danger Associated Molecular Patterns, which initiate an immune response. Withdrawal of the injurious agent and curtailing any pathogenic secondary immune response may allow spontaneous resolut...

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Autores principales: Richards, James A., Bucsaiova, Martina, Hesketh, Emily E., Ventre, Chiara, Henderson, Neil C., Simpson, Kenneth, Bellamy, Christopher O. C., Howie, Sarah E. M., Anderton, Stephen M., Hughes, Jeremy, Wigmore, Stephen J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4583453/
https://www.ncbi.nlm.nih.gov/pubmed/26406765
http://dx.doi.org/10.1371/journal.pone.0138688
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author Richards, James A.
Bucsaiova, Martina
Hesketh, Emily E.
Ventre, Chiara
Henderson, Neil C.
Simpson, Kenneth
Bellamy, Christopher O. C.
Howie, Sarah E. M.
Anderton, Stephen M.
Hughes, Jeremy
Wigmore, Stephen J.
author_facet Richards, James A.
Bucsaiova, Martina
Hesketh, Emily E.
Ventre, Chiara
Henderson, Neil C.
Simpson, Kenneth
Bellamy, Christopher O. C.
Howie, Sarah E. M.
Anderton, Stephen M.
Hughes, Jeremy
Wigmore, Stephen J.
author_sort Richards, James A.
collection PubMed
description BACKGROUND & AIMS: Acute liver injury is a clinically important pathology and results in the release of Danger Associated Molecular Patterns, which initiate an immune response. Withdrawal of the injurious agent and curtailing any pathogenic secondary immune response may allow spontaneous resolution of injury. The role B cells and Immunoglobulin M (IgM) play in acute liver injury is largely unknown and it was proposed that B cells and/or IgM would play a significant role in its pathogenesis. METHODS: Tissue from 3 models of experimental liver injury (ischemia-reperfusion injury, concanavalin A hepatitis and paracetamol-induced liver injury) and patients transplanted following paracetamol overdose were stained for evidence of IgM deposition. Mice deficient in B cells (and IgM) were used to dissect out the role B cells and/or IgM played in the development or resolution of injury. Serum transfer into mice lacking IgM was used to establish the role IgM plays in injury. RESULTS: Significant deposition of IgM was seen in the explanted livers of patients transplanted following paracetamol overdose as well as in 3 experimental models of acute liver injury (ischemia-reperfusion injury, concanavalin A hepatitis and paracetamol-induced liver injury). Serum transfer into IgM-deficient mice failed to reconstitute injury (p = 0.66), despite successful engraftment of IgM. Mice deficient in both T and B cells (RAG1-/-) mice (p<0.001), but not B cell deficient (μMT) mice (p = 0.93), were significantly protected from injury. Further interrogation with T cell deficient (CD3εKO) mice confirmed that the T cell component is a key mediator of sterile liver injury. Mice deficient in B cells and IgM mice did not have a significant delay in resolution following acute liver injury. DISCUSSION: IgM deposition appears to be common feature of both human and murine sterile liver injury. However, neither IgM nor B cells, play a significant role in the development of or resolution from acute liver injury. T cells appear to be key mediators of injury. In conclusion, the therapeutic targeting of IgM or B cells (e.g. with Rituximab) would have limited benefit in protecting patients from acute liver injury.
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spelling pubmed-45834532015-10-02 Acute Liver Injury Is Independent of B Cells or Immunoglobulin M Richards, James A. Bucsaiova, Martina Hesketh, Emily E. Ventre, Chiara Henderson, Neil C. Simpson, Kenneth Bellamy, Christopher O. C. Howie, Sarah E. M. Anderton, Stephen M. Hughes, Jeremy Wigmore, Stephen J. PLoS One Research Article BACKGROUND & AIMS: Acute liver injury is a clinically important pathology and results in the release of Danger Associated Molecular Patterns, which initiate an immune response. Withdrawal of the injurious agent and curtailing any pathogenic secondary immune response may allow spontaneous resolution of injury. The role B cells and Immunoglobulin M (IgM) play in acute liver injury is largely unknown and it was proposed that B cells and/or IgM would play a significant role in its pathogenesis. METHODS: Tissue from 3 models of experimental liver injury (ischemia-reperfusion injury, concanavalin A hepatitis and paracetamol-induced liver injury) and patients transplanted following paracetamol overdose were stained for evidence of IgM deposition. Mice deficient in B cells (and IgM) were used to dissect out the role B cells and/or IgM played in the development or resolution of injury. Serum transfer into mice lacking IgM was used to establish the role IgM plays in injury. RESULTS: Significant deposition of IgM was seen in the explanted livers of patients transplanted following paracetamol overdose as well as in 3 experimental models of acute liver injury (ischemia-reperfusion injury, concanavalin A hepatitis and paracetamol-induced liver injury). Serum transfer into IgM-deficient mice failed to reconstitute injury (p = 0.66), despite successful engraftment of IgM. Mice deficient in both T and B cells (RAG1-/-) mice (p<0.001), but not B cell deficient (μMT) mice (p = 0.93), were significantly protected from injury. Further interrogation with T cell deficient (CD3εKO) mice confirmed that the T cell component is a key mediator of sterile liver injury. Mice deficient in B cells and IgM mice did not have a significant delay in resolution following acute liver injury. DISCUSSION: IgM deposition appears to be common feature of both human and murine sterile liver injury. However, neither IgM nor B cells, play a significant role in the development of or resolution from acute liver injury. T cells appear to be key mediators of injury. In conclusion, the therapeutic targeting of IgM or B cells (e.g. with Rituximab) would have limited benefit in protecting patients from acute liver injury. Public Library of Science 2015-09-25 /pmc/articles/PMC4583453/ /pubmed/26406765 http://dx.doi.org/10.1371/journal.pone.0138688 Text en © 2015 Richards 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
Richards, James A.
Bucsaiova, Martina
Hesketh, Emily E.
Ventre, Chiara
Henderson, Neil C.
Simpson, Kenneth
Bellamy, Christopher O. C.
Howie, Sarah E. M.
Anderton, Stephen M.
Hughes, Jeremy
Wigmore, Stephen J.
Acute Liver Injury Is Independent of B Cells or Immunoglobulin M
title Acute Liver Injury Is Independent of B Cells or Immunoglobulin M
title_full Acute Liver Injury Is Independent of B Cells or Immunoglobulin M
title_fullStr Acute Liver Injury Is Independent of B Cells or Immunoglobulin M
title_full_unstemmed Acute Liver Injury Is Independent of B Cells or Immunoglobulin M
title_short Acute Liver Injury Is Independent of B Cells or Immunoglobulin M
title_sort acute liver injury is independent of b cells or immunoglobulin m
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4583453/
https://www.ncbi.nlm.nih.gov/pubmed/26406765
http://dx.doi.org/10.1371/journal.pone.0138688
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