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      SPARC/Osteonectin in Mineralized Tissue

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          Abstract

          Secreted protein acidic and rich in cysteine (SPARC/osteonectin/BM40) is one of the most abundant non-collagenous protein expressed in mineralized tissues. This review will focus on elucidating functional roles of SPARC in bone formation building upon results from non-mineralized cells and tissues, the phenotype of SPARC-null bones, and recent discoveries of human diseases with either dysregulated expression of SPARC or mutations in the gene encoding SPARC that give rise to bone pathologies. The capacity of SPARC to influence pathways involved in extracellular matrix assembly such as procollagen processing and collagen fibril formation as well as the capacity to influence osteoblast differentiation and osteoclast activity will be addressed. In addition, the potential for SPARC to regulate cross-linking of extracellular matrix proteins by members of the transglutaminase family of enzymes is explored. Elucidating defined biological functions of SPARC in terms of bone formation and turnover are critical. Further insight into specific cellular mechanisms involved in the formation and homeostasis of mineralized tissues will lead to a better understanding of disease progression.

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          Author and article information

          Journal
          9432592
          8496
          Matrix Biol
          Matrix Biol.
          Matrix biology : journal of the International Society for Matrix Biology
          0945-053X
          1569-1802
          16 March 2016
          03 February 2016
          May-Jul 2016
          01 May 2017
          : 52-54
          : 78-87
          Affiliations
          [1 ]Department of Oral Health Sciences, College of Dental Medicine, Medical University of South Carolina, Charleston, SC
          [2 ]Department of Medicine, Division of Cardiology, Medical University of South Carolina, Charleston, SC
          [3 ]Ralph H. Johnson Veterans Administration, VA Medical Center, Charleston, SC
          Article
          PMC5327628 PMC5327628 5327628 nihpa760740
          10.1016/j.matbio.2016.02.001
          5327628
          26851678
          30f5abf1-433d-474d-b220-cbd8403d1741
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