Measles Virus Nucleocapsid (MVNP) Gene Expression and RANK Receptor Signaling in Osteoclast Precursors, Osteoclast Inhibitors Peptide Therapy for Pagets Disease

Abstract

Pagers disease (PD) of bone occurs in 3-4% of population over the age of 50. We have identified expression of measles virus nucleocapsid transcripts in osteoclast (OCL) precursors and that MVNP expression induces pagetic phenotype in osteoclasts with increased bone resorption activity as seen in patients with Pagets disease. We previously cloned and identified osteoclast inhibitory peptide-I (01 P-I IhSca) which inhibits osteoclast formation and bone resorption. We hypothesize that MVNP expression in osteoclast precursors modulates RANK receptor signaling leading to Pagetic OCL development. OlP-I blocks these signaling events and inhibits MVNP induced osteoclastogenesis and elevated bone resorption activity. We demonstrated that MVNP increases TN F-alpha induced OCL differentiation and activation by increasing NF-kB signaling through increased expression of p62 and lKK-gama and increased MAPK signaling. Our results also suggest that MVNP%s effects on TN F-alpha signaling contribute to the increased OCL formation in PD. Furthermore expression of MVNP gene in OCL in vivo induces a pagetic-like phenotype. RANKL stimulation of OlP-I mice derived bone marrow cells resulted in significantly decreased osteoclast formation. Furthermore OlP-I transgenic mouse bones demonstrated an osteopetrotic phenotype. These data suggest that OlP-I is an important physiologic regulator of osteoclast development and bone resorption in vivo and may have therapeutic utility to control excess bone turnover in patients with Pagers disease.

Document Details

Document Type

Technical Report

Publication Date

Oct 01, 2007

Accession Number

ADA475186

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