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    Effects of receptor activator of NFκB (RANK) signaling blockade on fracture healing
    Wiley ; 2003
    In:  Journal of Orthopaedic Research Vol. 21, No. 4 ( 2003-07), p. 676-684
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    In: Journal of Orthopaedic Research, Wiley, Vol. 21, No. 4 ( 2003-07), p. 676-684
    Abstract: As dominant regulators of osteoclastogenesis and bone resorption, receptor activator of NFκB (RANK), receptor activator of NFκB ligand, and OPG have been identified as ideal drug targets for the treatment of metabolic bone disease. One concern regarding the therapeutic use of RANK signaling inhibitors is their effect on fracture healing. Therefore we tested if uncoupling and osteoclast depletion via RANK blockade affects callus formation, maturation and matrix remodeling, as well as union rates in a mouse tibia fracture model. Low dose (1 mg/kg i.p.) RANK:Fc therapy had no effect on callus formation, matrix maturation and remodeling, and resulted in 100% bony union by day 28. High dose RANK:Fc treatment (10 mg/kg i.p.) effectively eliminated osteoclasts at the fracture site on day 14, with no significant effects on fracture healing. When therapy was discontinued, normal numbers of osteoclasts were observed at the fracture site by day 28. However, continuous therapy resulted in a large osteopetrotic callus consisting of both mineralized and unmineralized matrix that was void of osteoclasts, but bony union was unaffected at day 28. We also evaluated this process in the complete absence of RANK signaling using RANK ‐/‐ mice. These animals exhibited significant radiographic and histologic evidence of callus formation, indicating that RANK signaling is not required for fracture callus formation. However, only 33% of RANK ‐/‐ animals formed bony unions compared to 100% of the osteopetrotic control mice. This defect was most likely a result of decreased blood flow, as evidenced by fewer blood vessels in the RANK ‐/‐ animals. Together, these data imply that osteoclast depletion via inhibition of RANK signaling is a viable option for the treatment of pathological bone loss since no adverse effects on fracture healing are observed when therapy is discontinued. © 2003 Orthopaedic Research Society. Published by Elsevier Science Ltd. All rights reserved.
    Type of Medium: Online Resource
    ISSN: 0736-0266 , 1554-527X
    URL: Article
    DOI: 10.1016/S0736-0266(03)00011-1
    Language: English
    Publisher: Wiley
    Publication Date: 2003
    detail.hit.zdb_id: 2050452-4
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