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      Transgenic Expression of Osteoactivin/gpnmb Enhances Bone Formation in Vivo and Osteoprogenitor Differentiation ex Vivo

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          Abstract

          Initial identification of osteoactivin (OA)/glycoprotein non-melanoma clone B (gpnmb) was demonstrated in an osteopetrotic rat model, where OA expression was increased 3-fold in mutant bones, compared to normal. OA mRNA and protein expression increase during active bone regeneration post-fracture, and primary rat osteoblasts show increased OA expression during differentiation in vitro. To further examine OA/gpnmb as an osteoinductive agent, we characterized the skeletal phenotype of transgenic mouse overexpressing OA/gpnmb under the CMV-promoter (OA-Tg). Western blot analysis showed increased OA/gpnmb in OA-Tg osteoblasts, compared to wild-type (WT). In OA-Tg mouse femurs versus WT littermates, micro-CT analysis showed increased trabecular bone volume and thickness, and cortical bone thickness; histomorphometry showed increased osteoblast numbers, bone formation and mineral apposition rates in OA-Tg mice; and biomechanical testing showed higher peak moment and stiffness. Given that OA/gpnmb is also over-expressed in osteoclasts in OA-Tg mice, we evaluated bone resorption by ELISA and histomorphometry, and observed decreased serum CTX-1 and RANK-L, and decreased osteoclast numbers in OA-Tg, compared to WT mice, indicating decreased bone remodeling in OA-Tg mice. The proliferation rate of OA-Tg osteoblasts in vitro was higher, compared to WT, as was alkaline phosphatase staining and activity, the latter indicating enhanced differentiation of OA-Tg osteoprogenitors. Quantitative RT-PCR analysis showed increased TGF-β1 and TGF-β receptors I and II expression in OA-Tg osteoblasts, compared to WT. Together, these data suggest that OA overexpression has an osteoinductive effect on bone mass in vivo and stimulates osteoprogenitor differentiation ex vivo.

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          Author and article information

          Journal
          0050222
          4586
          J Cell Physiol
          J. Cell. Physiol.
          Journal of cellular physiology
          0021-9541
          1097-4652
          17 July 2015
          January 2016
          01 January 2017
          : 231
          : 1
          : 72-83
          Affiliations
          [1 ]Department of Anatomy and Cell Biology, Temple University School of Medicine, Philadelphia, Pennsylvania
          [2 ]Department of Stem Cell Biology and Regenerative Medicine, Lerner Research Institute, Cleveland Clinic, Cleveland, Ohio
          [3 ]Department of Anatomy and Neurobiology, Northeast Ohio Medical University (NEOMED), Rootstown, Ohio
          [4 ]School of Biomedical Sciences, Kent State University, Kent, Ohio
          [5 ]Department of Kinesiology, California State University, East Bay, Hayward, California
          [6 ]School of Theoretical and Applied Science (TAS), Ramapo College of New Jersey, Mahwah, New Jersey
          Author notes
          [* ]Corresponding Author: Fayez F. Safadi, Ph.D., Department of Anatomy and Neurobiology, Northeast Ohio Medical University (NEOMED), 4209 State Rt, 44, Rootstown, OH 44224, Phone: 330-325-6619, Fax: 330-325-5916, fayez.safadi@ 123456neomed.edu
          Article
          PMC4586905 PMC4586905 4586905 nihpa707875
          10.1002/jcp.25020
          4586905
          25899717
          001085fc-06cf-449b-81e2-0bc62d336113
          History
          Categories
          Article

          Osteoblast differentiation,Bone,Osteoactivin/Gpnmb,Growth factors

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