Osteomodulin downregulation is associated with osteoarthritis development

Author:

Zappia Jérémie,Tong Qiao,Van der Cruyssen Renée,Cornelis Frederique M. F.,Lambert Cécile,Pinto Coelho Tiago,Grisart Juliane,Kague ErikaORCID,Lories Rik J.,Muller MarcORCID,Elewaut Dirk,Hammond Chrissy L.,Sanchez Christelle,Henrotin Yves

Abstract

AbstractAbnormal subchondral bone remodeling leading to sclerosis is a main feature of osteoarthritis (OA), and osteomodulin (OMD), a proteoglycan involved in extracellular matrix mineralization, is associated with the sclerotic phenotype. However, the functions of OMD remain poorly understood, specifically in vivo. We used Omd knockout and overexpressing male mice and mutant zebrafish to study its roles in bone and cartilage metabolism and in the development of OA. The expression of Omd is deeply correlated with bone and cartilage microarchitectures affecting the bone volume and the onset of subchondral bone sclerosis and spontaneous cartilage lesions. Mechanistically, OMD binds to RANKL and inhibits osteoclastogenesis, thus controlling the balance of bone remodeling. In conclusion, OMD is a key factor in subchondral bone sclerosis associated with OA. It participates in bone and cartilage homeostasis by acting on the regulation of osteoclastogenesis. Targeting OMD may be a promising new and personalized approach for OA.

Funder

Versus Arthritis Grant Reference Number 21937

Fonds De La Recherche Scientifique - FNRS

Publisher

Springer Science and Business Media LLC

Subject

Physiology,Histology,Endocrinology, Diabetes and Metabolism

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