Oxidative modification of type II collagen differentially affects its arthritogenic and tolerogenic capacity in experimental arthritis

Marcinkiewicz, J.; Biedron, R.; Maresz, K.; Kwasny-Krochin, B.; Bobek, M.; Kontny, E.; Maslinski, W.; Chain, B.

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Artykuł - szczegóły

Czasopismo

Archivum Immunologiae et Therapiae Experimentalis

2004 | 52 | 4 | 284-291

Tytuł artykułu

Oxidative modification of type II collagen differentially affects its arthritogenic and tolerogenic capacity in experimental arthritis

Autorzy

J. Marcinkiewicz , R. Biedron , K. Maresz , B. Kwasny-Krochin , M. Bobek , E. Kontny , W. Maslinski , B. Chain

Warianty tytułu

Języki publikacji

Abstrakty

Oxidative modification of proteins affects their biological properties. Previously we have shown that hypochlorite (HOCl), the product of activated neutrophils, enhances protein immunogenecity. Collagen type II, a primary component of cartilage, is commonly used in the induction of arthritis in animals (CIA). The aim of this study was to examine whether HOCl may affect immunogenic, tolerogenic, and arthritogenic properties of collagen. DBA/J mice were injected with either native (CNAT) or chlorinated collagen (CHOCl) to induce arthritis. The effect of chlorination on collagen properties was measured by evaluation of incidence and severity of CIA. Moreover, the concentration of serum anti-collagen IgG antibodies and myeloperoxidase (MPO) activity in inflamed joints was determined. Mice immunized with CNAT in adjuvant developed arthritis (CIA) with an incidence of 69%. CNAT also exerted tolerogenic properties when injected intravenously either before or shortly after primary immunization, resulting in decreased incidence and severity of CIA, reduced MPO activity in inflamed joints, and lowered serum levels of anti-CNAT IgG antibodies. Chlorination of collagen significantly diminished its ability to induce CIA and to trigger generation of anti-CNAT IgG antibodies. Interestingly, chlorination did not affect tolerogenic properties of collagen administered prior to primary immunization with CNAT. These results suggest that chlorination of collagen may selectively affect functional epitopes of collagen. It is likely that in inflamed joints, neutrophil-derived HOCl, in some circumstances, will destroy arthritogenic and immunogenic B cell epitopes, while regulatory T cell epitopes will be preserved.

Słowa kluczowe

ARTHRITIS COLLAGEN MOUSE NEUTROPHIL PROTEIN OXIDATION

Wydawca

Czasopismo

Archivum Immunologiae et Therapiae Experimentalis

Rocznik

2004

Tom

Numer

Strony

284-291

Opis fizyczny

Twórcy

autor

J. Marcinkiewicz

autor

R. Biedron

autor

K. Maresz

autor

B. Kwasny-Krochin

autor

M. Bobek

autor

E. Kontny

autor

W. Maslinski

autor

B. Chain

Bibliografia

Typ dokumentu

ARTICLE

Bibliografia

Janusz Marcinkiewicz, Department of Immunology, Jagiellonian University Medical College, Czysta 18, 31-121 Krakow, Poland

Identyfikatory

Identyfikator YADDA

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