| Literature DB >> 27798154 |
Casimiro L Gigliotti1, Elena Boggio1, Nausicaa Clemente1, Yogesh Shivakumar1, Erika Toth1, Daniele Sblattero1, Patrizia D'Amelio2, Giovanni C Isaia2, Chiara Dianzani3, Junji Yagi4, Josè M Rojo5, Annalisa Chiocchetti1, Renzo Boldorini1, Michela Bosetti6, Umberto Dianzani7.
Abstract
Osteoblasts, osteocytes, and osteoclasts (OCs) are involved in the bone production and resorption, which are crucial in bone homeostasis. OC hyperactivation plays a role in the exaggerated bone resorption of diseases such as osteoporosis, rheumatoid arthritis, and osteolytic tumor metastases. This work stems from the finding that OCs can express B7h (ICOS-Ligand), which is the ligand of the ICOS T cell costimulatory molecule. Because recent reports have shown that, in endothelial, dendritic, and tumor cells, B7h triggering modulates several activities of these cells, we analyzed the effect of B7h triggering by recombinant ICOS-Fc on OC differentiation and function. The results showed that ICOS-Fc inhibits RANKL-mediated differentiation of human monocyte-derived OC-like cells (MDOCs) by inhibiting the acquirement of the OC morphology, the CD14- cathepsin K+ phenotype, and the expression of tartrate-resistant acid phosphatase, OSCAR, NFATc1, and DC-STAMP. Moreover, ICOS-Fc induces a reversible decrease in the sizes of cells and nuclei and cathepsin K expression in mature MDOCs. Finally, ICOS-Fc inhibits the osteolytic activities of MDOCs in vitro and the development of bone loss in ovariectomized or soluble RANKL-treated mice. These findings open a novel field in the pharmacological use of agonists and antagonists of the ICOS-B7h system.Entities:
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Year: 2016 PMID: 27798154 DOI: 10.4049/jimmunol.1600424
Source DB: PubMed Journal: J Immunol ISSN: 0022-1767 Impact factor: 5.422