ORIGINAL ARTICLE: Detection, epitope-mapping and function of anti-Fas autoantibody in patients with silicosis

ORIGINAL ARTICLE: Detection, epitope-mapping and function of anti-Fas autoantibody in patients with silicosis

Dysregulation of apoptosis through the Fas-Fas ligand pathway is associated with the onset of autoimmune disease. Since autoantibodies directed against unknown antigens are present in the sera of these patients, sera samples were examined for the presence of autoantibodies directed against the Fas m...

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Veröffentlicht in:Immunology 2005-09, Vol.116 (1), p.21-29
Hauptverfasser: Takata-Tomokuni, Akiko, Ueki, Ayako, Shiwa, Mieko, Isozaki, Yumika, Hatayama, Tamayo, Katsuyama, Hironobu, Hyodoh, Fuminori, Fujimoto, Wataru, Ueki, Hiroaki, Kusaka, Masayasu, Arikuni, Hisashi, Otsuki, Takemi
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container_issue 1
container_start_page 21
container_title Immunology
container_volume 116
creator Takata-Tomokuni, Akiko
Ueki, Ayako
Shiwa, Mieko
Isozaki, Yumika
Hatayama, Tamayo
Katsuyama, Hironobu
Hyodoh, Fuminori
Fujimoto, Wataru
Ueki, Hiroaki
Kusaka, Masayasu
Arikuni, Hisashi
Otsuki, Takemi
description Dysregulation of apoptosis through the Fas-Fas ligand pathway is associated with the onset of autoimmune disease. Since autoantibodies directed against unknown antigens are present in the sera of these patients, sera samples were examined for the presence of autoantibodies directed against the Fas molecule. Using Western blotting and a ProteinChip analysis, autoantibodies against Fas were detected in patients with silicosis, systemic lupus erythematosus (SLE) and systemic sclerosis (SSc), and weakly detected in healthy individuals. Using epitope mapping employing 12-amino-acid polypeptides with the SPOTs system, a minimum of four epitopes and a maximum of 10 epitopes were found. Several amino acid residues involved in binding FasL, such as C66, R87, L90, E93 and H126, were presented within the epitopes. Serum containing a large amount of anti-Fas autoantibody from silicosis patients inhibited the growth of a Fas-expressing human cell line, but did not inhibit the growth of a low Fas-expresser nor a Fas-expresser in which the Fas gene had been silenced by small interference RNA. All epitopes in the intracellular region of Fas were located in the death domain. The possible roles of anti-Fas autoantibody detected in healthy volunteers and patients with silicosis or autoimmune diseases are discussed here.
doi_str_mv 10.1111/j.1365-2567.2005.02192.x
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title ORIGINAL ARTICLE: Detection, epitope-mapping and function of anti-Fas autoantibody in patients with silicosis
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