Over-expression of the decoy receptor 3 (DcR3) gene in peripheral blood mononuclear cells (PBMC) derived from silicosis patients

Otsuki, Takemi; Tomokuni, A; Sakaguchi, Haruko; Aikoh, T; Matsuki, Takakazu; Isozaki, Yumika; Hyodoh, Fuminori; Ueki, Hiroaki; Kusaka, Masayasu; Kita, Shoichi; Ueki, Ayako

doi:10.1046/j.1365-2249.2000.01132.x

Cited by 65 publications

(49 citation statements)

References 33 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…DcR3 is overexpressed in malignant tumors arising from lung, colon, glioma, and gastrointestinal track; virus-associated lymphoma (1, 4 -7); as well as the PBMC of silicosis patients (8). In addition, high serum levels of DcR3 have been detected in many cancer patients (9) and are associated with poor prognoses (6).…”

Section: Ecoy Receptor 3 (Dcr3)mentioning

confidence: 99%

The Glycosaminoglycan-Binding Domain of Decoy Receptor 3 Is Essential for Induction of Monocyte Adhesion

Chang¹,

Chan²,

Jackson

et al. 2006

The Journal of Immunology

View full text Add to dashboard Cite

Decoy receptor 3 (DcR3), a soluble receptor for Fas ligand, LIGHT (homologous to lymphotoxins shows inducible expression and competes with HSV glycoprotein D for herpes virus entry mediator, a receptor expressed by T lymphocytes), and TNF-like molecule 1A, is highly expressed in cancer cells and in tissues affected by autoimmune disease. DcR3.Fc has been shown to stimulate cell adhesion and to modulate cell activation and differentiation by triggering multiple signaling cascades that are independent of its three known ligands. In this study we found that DcR3.Fc-induced cell adhesion was inhibited by heparin and heparan sulfate, and that DcR3.Fc was unable to bind Chinese hamster ovary K1 mutants defective in glycosaminoglycan (GAG) synthesis. Furthermore, the negatively charged, sulfated GAGs of cell surface proteoglycans, but not their core proteins, were identified as the binding sites for DcR3.Fc. A potential GAG-binding site was found in the C-terminal region of DcR3, and the mutation of three basic residues, i.e., K256, R258, and R259, to alanines abolished its ability to trigger cell adhesion. Moreover, a fusion protein comprising the GAG-binding region of DcR3 with an Fc fragment (DcR3_HBD.Fc) has the same effect as DcR3.Fc in activating protein kinase C and inducing cell adhesion. Compared with wild-type THP-1 cells, cell adhesion induced by DcR3.Fc was significantly reduced in both CD44v3 and syndecan-2 knockdown THP-1 cells. Therefore, we propose a model in which DcR3.Fc may bind to and cross-link proteoglycans to induce monocyte adhesion.

show abstract

Section: Ecoy Receptor 3 (Dcr3)mentioning

confidence: 99%

The Glycosaminoglycan-Binding Domain of Decoy Receptor 3 Is Essential for Induction of Monocyte Adhesion

Chang¹,

Chan²,

Jackson

et al. 2006

The Journal of Immunology

View full text Add to dashboard Cite

show abstract

“…We found that dysregulation of the Fas-mediated apoptotic pathway might play an important role in the pathogenesis of the immunological abnormalities found in silicosis patients 7,8,[17][18][19] . Therefore, it is suggested that the genesis of anti-topo I autoantibodies is associated with the abnormalities of apoptosis-related molecules in silicosis patients.…”

Section: Discussionmentioning

confidence: 84%

“…In addition, silicosis patients in the anti-topo I (+) group showed inverse correlations between the serum sFas levels and PaCO 2 values, although patients in the anti-topo I (−) group did not. Moreover, our previous studies 7,19) on dysregulation of the Fas/FasL pathway showed that the same series of patients with silicosis or SLE showed higher serum sFas levels and over-expres- sion of the decoy receptor 3 gene in peripheral blood mononuclear cells, while SSc patients did not. These findings suggest that the genesis of anti-topo I autoantibodies is related to pulmonary involvement or lung fibrosis associated with progression of silicosis, and that it may have little association with dysregulation of the Fas-mediated apoptotic pathway.…”

Section: Discussionmentioning

confidence: 91%

Detection of anti-topoisomerase I autoantibody in patients with silicosis

Tomokuni

Otsuki

Sakaguchi

et al. 2002

Environ Health Prev Med

View full text Add to dashboard Cite

Objectives: The aim of this study was to detect anti-topoisomerase l (anti-topo I) autoantibodies, which are known to be limited in systemic sclerosis patients, in silicosis patients with no clinical symptoms of autoimmune disease.Methods: Serum anti-topo I autoantibodies were detected using ELISA. Differences in clinical parameters between patients with and without anti-topo I autoantibodies were analyzed.Results: Seven of 69 patients had anti-topo I autoantibodies. These 7 patients showed elevated PaCO 2 values (P=0.0212), and inverse correlations between serum soluble Fas levels and PaCO 2 values were found.Conclusion: Anti-topo I autoantibodies were detected in 10.1% of silicosis patients without any clinical symptoms of autoimmune disease. The findings here suggest that the genesis of anti-topo l autoantibodies might be related to pulmonary involvement or lung fibrosis associated with progression of silicosis.

show abstract

“…The weaker membrane Fas expressers (among lymphocytes) were identified to be weaker fas message expressers . The gene expression levels of extracellular inhibitor competing membrane Fas-FasL binding such as sFas, decoy receptor 3 (DCR3), and other alternatively spliced variants of the fas gene were higher in peripheral blood mononuclear cells (PBMC) from SILs than HVs (Otsuki, 2000a(Otsuki, , 2000b. The intracellular apoptosis-inhibitory genes including i-flice, sentrin, survivine and icad showed a lower expression in PBMC from SILs than HDs (Guo, 2001;Otsuki, 2000c).…”

Section: Alteration Of Fas/cd95 and Its Related Molecules In Silsmentioning

confidence: 99%