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Sundeep Khosla, Jennifer J. Westendorf, Merry Jo Oursler
J Clin Invest. 2008;
118(2):421
doi:10.1172/JCI33612
Abstract |
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A
n important, unfilled clinical need is the development of new approaches to improve fracture healing and to treat osteoporosis by increasing bone mass. Recombinant forms of bone morphogenetic protein 2 (BMP2) and BMP7 are FDA approved to promote spinal fusion and fracture healing, respectively, and the first FDA-approved anabolic drug for osteoporosis, parathyroid hormone, increases bone mass when administered intermittently but can only be given to patients in the US for two years. As we discuss here, the tremendous explosion over the last two decades in our fundamental understanding of the mechanisms of bone remodeling has led to the prospect of mechanism-based anabolic therapies for bone disorders.
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Citations to this article
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(56)
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Bioorganic & Medicinal Chemistry Letters
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The bone and beyond: A shift in calcium
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Nat Med
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Novel oxysterols have pro-osteogenic and anti-adipogenic effects in vitro and induce spinal fusion in vivo
Jared S. Johnson, Vicente Meliton, Woo Kyun Kim, Kwang-Bok Lee, Jeffrey C. Wang, KhanhLinh Nguyen, Dongwon Yoo, Michael E. Jung, Elisa Atti, Sotirios Tetradis, Renata C. Pereira, Clara Magyar, Taya Nargizyan, Theodore J. Hahn, Francine Farouz, Scott Thies, Farhad Parhami
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The unitary model for estrogen deficiency and the pathogenesis of osteoporosis: Is a revision needed?
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Ultrasound therapy modulates osteocalcin expression during bone repair in rats
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