| Literature DB >> 33020147 |
Marina A Korn1, Heike Schmitt1, Sieglinde Angermüller1, David Chambers1, Michaela Seeling1, Uwe T Lux2, Stefanie Brey1, Dmytro Royzman3, Christin Brückner1, Vanessa Popp4, Elena Percivalle4, Tobias Bäuerle4, Elisabeth Zinser3, Thomas H Winkler1, Alexander Steinkasserer3, Falk Nimmerjahn1, Lars Nitschke5.
Abstract
Siglec-15 is a conserved sialic acid-binding Ig-like lectin, which is expressed on osteoclasts. Deficiency of Siglec-15 leads to an impaired osteoclast development, resulting in a mild osteopetrotic phenotype. The role of Siglec-15 in arthritis is still largely unclear. To address this, we generated Siglec-15 knockout mice and analyzed them in a mouse arthritis model. We could show that Siglec-15 is directly involved in pathologic bone erosion in the K/BxN serum-transfer arthritis model. Histological analyses of joint destruction provided evidence for a significant reduction in bone erosion area and osteoclast numbers in Siglec-15-/- mice, whereas the inflammation area and cartilage destruction was comparable to wild-type mice. Thus, Siglec-15 on osteoclasts has a crucial function for bone erosion during arthritis. In addition, we generated a new monoclonal anti-Siglec-15 Ab to clarify its expression pattern on immune cells. Whereas this Ab demonstrated an almost exclusive Siglec-15 expression on murine osteoclasts and hardly any other expression on various other immune cell types, human Siglec-15 was more broadly expressed on human myeloid cells, including human osteoclasts. Taken together, our findings show a role of Siglec-15 as a regulator of pathologic bone resorption in arthritis and highlight its potential as a target for future therapies, as Siglec-15 blocking Abs are available.Entities:
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Year: 2020 PMID: 33020147 DOI: 10.4049/jimmunol.2000472
Source DB: PubMed Journal: J Immunol ISSN: 0022-1767 Impact factor: 5.422