Bone morphogenetic protein 2 enhances PGE 2-stimulated osteoclast formation in murine bone marrow cultures

Abstract

Bone morphogenetic protein 2 (BMP-2) is used clinically to stimulate bone formation and accelerate fracture repair. Adding prostaglandin (PG) E 2 or PGE 2 receptor agonists to BMP-2 has been proposed to improve BMP-2 efficacy. However, this may enhance bone resorption, since PGE 2 can increase receptor activator of NF-κB ligand (RANKL) expression and decrease osteoprotegerin (OPG) expression in osteoblasts, and the RANKL:OPG ratio is critical for osteoclast formation. We used bone marrow (BM) cultures and BM macrophage (BMM) cultures from outbred CD1 mice to examine effects on osteoclast formation of BMP-2 and PGE 2. In BM cultures, which contain both osteoblastic and osteoclastic lineage cells, BMP-2 (100 ng/ml) alone did not increase osteoclast formation but enhanced the peak response to PGE 2 by 1.6–9.6-fold. In BMM cultures, which must be treated with RANKL because they do not contain osteoblastic cells, BMP-2 did not increase osteoclast formation, with or without PGE 2. Our results suggest that BMP-2 can increase osteoclast formation in response to PGE 2 by increasing the RANKL:OPG ratio in osteoblasts, which may have therapeutic implications for the use of BMP-2.