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Osteoclast Derivation from Mouse Bone Marrow
Authors:Ruth Tevlin  Adrian McArdle  Charles K.F. Chan  John Pluvinage  Graham G. Walmsley  Taylor Wearda  Owen Marecic  Michael S. Hu  Kevin J. Paik  Kshemendra Senarath-Yapa  David A. Atashroo  Elizabeth R. Zielins  Derrick C. Wan  Irving L. Weissman  Michael T. Longaker
Affiliation:1.Hagey Laboratory for Pediatric Regenerative Medicine, Division of Plastic and Reconstructive Surgery, Department of Surgery, Stanford University School of Medicine;2.Institute for Stem Cell Biology and Regenerative Medicine, Stanford University
Abstract:Osteoclasts are highly specialized cells that are derived from the monocyte/macrophage lineage of the bone marrow. Their unique ability to resorb both the organic and inorganic matrices of bone means that they play a key role in regulating skeletal remodeling. Together, osteoblasts and osteoclasts are responsible for the dynamic coupling process that involves both bone resorption and bone formation acting together to maintain the normal skeleton during health and disease.As the principal bone-resorbing cell in the body, changes in osteoclast differentiation or function can result in profound effects in the body. Diseases associated with altered osteoclast function can range in severity from lethal neonatal disease due to failure to form a marrow space for hematopoiesis, to more commonly observed pathologies such as osteoporosis, in which excessive osteoclastic bone resorption predisposes to fracture formation.An ability to isolate osteoclasts in high numbers in vitro has allowed for significant advances in the understanding of the bone remodeling cycle and has paved the way for the discovery of novel therapeutic strategies that combat these diseases. Here, we describe a protocol to isolate and cultivate osteoclasts from mouse bone marrow that will yield large numbers of osteoclasts.
Keywords:Cellular Biology   Issue 93   osteoclast   RANKL   culture   resorption assay   bone remodeling   bone turnover   skeletal homeostasis
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