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Marcelo Napimoga, Elizabeth Martinez, Daiane Peruzzo, Vanessa Carregaro, Vera de Araújo, M Weitzmann, Expression of secreted osteoclastogenic factor of activated T cells (SOFAT) by T- and B-lineage cells may contribute significantly to bone loss in periodontitis. (CCR3P.221), The Journal of Immunology, Volume 192, Issue Supplement_1, May 2014, Page 115.18, https://doi.org/10.4049/jimmunol.192.Supp.115.18
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Abstract
A novel T cell-secreted cytokine, termed secreted osteoclastogenic factor of activated T cells (SOFAT), that induces osteoclastic bone resorption in a RANKL-independent manner, has recently been described. We have previously reported that SOFAT is highly expressed in gingival tissues of patients with chronic periodontitis (CP) suggesting a putative role in the bone loss associated with CP. Here we characterized the cell types producing SOFAT in CP. Gingival tissues were biopsied from subjects without periodontal disease (n=5) and patients with CP (n=5) and SOFAT quantified by immunohistochemistry and immunofluorescence staining. Our data reveal marked SOFAT staining in CP that was predominantly associated with the lymphocytic infiltration of gingival tissues. Interestingly, besides CD3+ T cells, B-lineage cells including plasma cells also exhibited strong staining for SOFAT. Because SOFAT has not previously been reported in B-linage cells, we further purified splenic T cells and B cells from Balb/c mice and activated them using LPS or CD3/CD28 antibodies respectively. SOFAT was quantified by RT-qPCR and revealed significant induction of SOFAT expression in both activated T cells and B cells in comparison to unstimulated cells. Our data support a putative role of SOFAT in the bone loss associated with chronic periodontitis and further demonstrates for the first time that in addition to T cells, B-linage cells may also be a significant source of SOFAT in inflammatory states.
