NADPH-oxidase-driven oxygen radical production determines chondrocyte death and partly regulates metalloproteinase-mediated cartilage matrix degradation during interferon-γ-stimulated immune complex arthritis

In previous studies we have found that FcγRI determines chondrocyte death and matrix metalloproteinase (MMP)-mediated cartilage destruction during IFN-γ-regulated immune complex arthritis (ICA). Binding of immune complexes (ICs) to FcγRI leads to the prominent production of oxygen radicals. In the p...

Descripción completa

Detalles Bibliográficos
Autores principales: van Lent, Peter LEM, Nabbe, Karin CAM, Blom, Arjen B, Sloetjes, Annet, Holthuysen, Astrid EM, Kolls, Jay, Van De Loo, Fons AJ, Holland, Steven M, Van Den Berg, Wim B
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2005
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1175041/
https://www.ncbi.nlm.nih.gov/pubmed/15987491
http://dx.doi.org/10.1186/ar1760
_version_ 1782124496949346304
author van Lent, Peter LEM
Nabbe, Karin CAM
Blom, Arjen B
Sloetjes, Annet
Holthuysen, Astrid EM
Kolls, Jay
Van De Loo, Fons AJ
Holland, Steven M
Van Den Berg, Wim B
author_facet van Lent, Peter LEM
Nabbe, Karin CAM
Blom, Arjen B
Sloetjes, Annet
Holthuysen, Astrid EM
Kolls, Jay
Van De Loo, Fons AJ
Holland, Steven M
Van Den Berg, Wim B
author_sort van Lent, Peter LEM
collection PubMed
description In previous studies we have found that FcγRI determines chondrocyte death and matrix metalloproteinase (MMP)-mediated cartilage destruction during IFN-γ-regulated immune complex arthritis (ICA). Binding of immune complexes (ICs) to FcγRI leads to the prominent production of oxygen radicals. In the present study we investigated the contribution of NADPH-oxidase-driven oxygen radicals to cartilage destruction by using p47phox(-/- )mice lacking a functional NADPH oxidase complex. Induction of a passive ICA in the knee joints of p47phox(-/- )mice resulted in a significant elevation of joint inflammation at day 3 when compared with wild-type (WT) controls as studied by histology. However, when IFN-γ was overexpressed by injection of adenoviral IFN-γ in the knee joint before ICA induction, a similar influx of inflammatory cells was found at days 3 and 7, comprising mainly macrophages in both mouse strains. Proteoglycan depletion from the cartilage layers of the knee joints in both groups was similar at days 3 and 7. Aggrecan breakdown in cartilage caused by MMPs was further studied by immunolocalisation of MMP-mediated neoepitopes (VDIPEN). VDIPEN expression in the cartilage layers of arthritic knee joints was markedly lower (between 30 and 60%) in IFN-γ-stimulated arthritic p47phox(-/- )mice at day 7 than in WT controls, despite significant upregulation of mRNA levels of various MMPs such as MMP-3, MMP-9, MMP-12 and MMP-13 in synovia and MMP-13 in cartilage layers as measured with quantitative RT-PCR. The latter observation suggests that oxygen radicals are involved in the activation of latent MMPs. Chondrocyte death, determined as the percentage of empty lacunae in articular cartilage, ranged between 20 and 60% at day 3 and between 30 and 80% at day 7 in WT mice, and was completely blocked in p47phox(-/- )mice at both time points. FcγRI mRNA expression was significantly lower, and FcγRII and FcγRIII were higher, in p47phox(-/- )mice than in controls. NADPH-oxidase-driven oxygen radical production determines chondrocyte death and aggravates MMP-mediated cartilage destruction during IFN-γ-stimulated IC-mediated arthritis. Upregulation of FcγRI by oxygen radicals may contribute to cartilage destruction.
format Text
id pubmed-1175041
institution National Center for Biotechnology Information
language English
publishDate 2005
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-11750412005-07-14 NADPH-oxidase-driven oxygen radical production determines chondrocyte death and partly regulates metalloproteinase-mediated cartilage matrix degradation during interferon-γ-stimulated immune complex arthritis van Lent, Peter LEM Nabbe, Karin CAM Blom, Arjen B Sloetjes, Annet Holthuysen, Astrid EM Kolls, Jay Van De Loo, Fons AJ Holland, Steven M Van Den Berg, Wim B Arthritis Res Ther Research Article In previous studies we have found that FcγRI determines chondrocyte death and matrix metalloproteinase (MMP)-mediated cartilage destruction during IFN-γ-regulated immune complex arthritis (ICA). Binding of immune complexes (ICs) to FcγRI leads to the prominent production of oxygen radicals. In the present study we investigated the contribution of NADPH-oxidase-driven oxygen radicals to cartilage destruction by using p47phox(-/- )mice lacking a functional NADPH oxidase complex. Induction of a passive ICA in the knee joints of p47phox(-/- )mice resulted in a significant elevation of joint inflammation at day 3 when compared with wild-type (WT) controls as studied by histology. However, when IFN-γ was overexpressed by injection of adenoviral IFN-γ in the knee joint before ICA induction, a similar influx of inflammatory cells was found at days 3 and 7, comprising mainly macrophages in both mouse strains. Proteoglycan depletion from the cartilage layers of the knee joints in both groups was similar at days 3 and 7. Aggrecan breakdown in cartilage caused by MMPs was further studied by immunolocalisation of MMP-mediated neoepitopes (VDIPEN). VDIPEN expression in the cartilage layers of arthritic knee joints was markedly lower (between 30 and 60%) in IFN-γ-stimulated arthritic p47phox(-/- )mice at day 7 than in WT controls, despite significant upregulation of mRNA levels of various MMPs such as MMP-3, MMP-9, MMP-12 and MMP-13 in synovia and MMP-13 in cartilage layers as measured with quantitative RT-PCR. The latter observation suggests that oxygen radicals are involved in the activation of latent MMPs. Chondrocyte death, determined as the percentage of empty lacunae in articular cartilage, ranged between 20 and 60% at day 3 and between 30 and 80% at day 7 in WT mice, and was completely blocked in p47phox(-/- )mice at both time points. FcγRI mRNA expression was significantly lower, and FcγRII and FcγRIII were higher, in p47phox(-/- )mice than in controls. NADPH-oxidase-driven oxygen radical production determines chondrocyte death and aggravates MMP-mediated cartilage destruction during IFN-γ-stimulated IC-mediated arthritis. Upregulation of FcγRI by oxygen radicals may contribute to cartilage destruction. BioMed Central 2005 2005-05-20 /pmc/articles/PMC1175041/ /pubmed/15987491 http://dx.doi.org/10.1186/ar1760 Text en Copyright © 2005 van Lent et al.; licensee BioMed Central Ltd.
spellingShingle Research Article
van Lent, Peter LEM
Nabbe, Karin CAM
Blom, Arjen B
Sloetjes, Annet
Holthuysen, Astrid EM
Kolls, Jay
Van De Loo, Fons AJ
Holland, Steven M
Van Den Berg, Wim B
NADPH-oxidase-driven oxygen radical production determines chondrocyte death and partly regulates metalloproteinase-mediated cartilage matrix degradation during interferon-γ-stimulated immune complex arthritis
title NADPH-oxidase-driven oxygen radical production determines chondrocyte death and partly regulates metalloproteinase-mediated cartilage matrix degradation during interferon-γ-stimulated immune complex arthritis
title_full NADPH-oxidase-driven oxygen radical production determines chondrocyte death and partly regulates metalloproteinase-mediated cartilage matrix degradation during interferon-γ-stimulated immune complex arthritis
title_fullStr NADPH-oxidase-driven oxygen radical production determines chondrocyte death and partly regulates metalloproteinase-mediated cartilage matrix degradation during interferon-γ-stimulated immune complex arthritis
title_full_unstemmed NADPH-oxidase-driven oxygen radical production determines chondrocyte death and partly regulates metalloproteinase-mediated cartilage matrix degradation during interferon-γ-stimulated immune complex arthritis
title_short NADPH-oxidase-driven oxygen radical production determines chondrocyte death and partly regulates metalloproteinase-mediated cartilage matrix degradation during interferon-γ-stimulated immune complex arthritis
title_sort nadph-oxidase-driven oxygen radical production determines chondrocyte death and partly regulates metalloproteinase-mediated cartilage matrix degradation during interferon-γ-stimulated immune complex arthritis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1175041/
https://www.ncbi.nlm.nih.gov/pubmed/15987491
http://dx.doi.org/10.1186/ar1760
work_keys_str_mv AT vanlentpeterlem nadphoxidasedrivenoxygenradicalproductiondetermineschondrocytedeathandpartlyregulatesmetalloproteinasemediatedcartilagematrixdegradationduringinterferongstimulatedimmunecomplexarthritis
AT nabbekarincam nadphoxidasedrivenoxygenradicalproductiondetermineschondrocytedeathandpartlyregulatesmetalloproteinasemediatedcartilagematrixdegradationduringinterferongstimulatedimmunecomplexarthritis
AT blomarjenb nadphoxidasedrivenoxygenradicalproductiondetermineschondrocytedeathandpartlyregulatesmetalloproteinasemediatedcartilagematrixdegradationduringinterferongstimulatedimmunecomplexarthritis
AT sloetjesannet nadphoxidasedrivenoxygenradicalproductiondetermineschondrocytedeathandpartlyregulatesmetalloproteinasemediatedcartilagematrixdegradationduringinterferongstimulatedimmunecomplexarthritis
AT holthuysenastridem nadphoxidasedrivenoxygenradicalproductiondetermineschondrocytedeathandpartlyregulatesmetalloproteinasemediatedcartilagematrixdegradationduringinterferongstimulatedimmunecomplexarthritis
AT kollsjay nadphoxidasedrivenoxygenradicalproductiondetermineschondrocytedeathandpartlyregulatesmetalloproteinasemediatedcartilagematrixdegradationduringinterferongstimulatedimmunecomplexarthritis
AT vandeloofonsaj nadphoxidasedrivenoxygenradicalproductiondetermineschondrocytedeathandpartlyregulatesmetalloproteinasemediatedcartilagematrixdegradationduringinterferongstimulatedimmunecomplexarthritis
AT hollandstevenm nadphoxidasedrivenoxygenradicalproductiondetermineschondrocytedeathandpartlyregulatesmetalloproteinasemediatedcartilagematrixdegradationduringinterferongstimulatedimmunecomplexarthritis
AT vandenbergwimb nadphoxidasedrivenoxygenradicalproductiondetermineschondrocytedeathandpartlyregulatesmetalloproteinasemediatedcartilagematrixdegradationduringinterferongstimulatedimmunecomplexarthritis

Ejemplares similares