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      NG2 Is a Major Chondroitin Sulfate Proteoglycan Produced after Spinal Cord Injury and Is Expressed by Macrophages and Oligodendrocyte Progenitors

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      The Journal of Neuroscience
      Society for Neuroscience

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          Abstract

          <p class="first" id="d2144783e152">Several extracellular matrix (ECM) molecules have been identified as potent inhibitors of neurite outgrowth <i>in vitro</i> and are believed to limit axonal growth after CNS injury. Recent studies have shown that different members of the chondroitin sulfate proteoglycan (CSPG) class of putatively inhibitory ECM molecules are expressed after a number of CNS injuries. The purpose of this study was to evaluate the relative amounts of individual CSPGs expressed after spinal cord injury (SCI) and identify their cells of origin. Evaluation of total soluble CSPGs 2 weeks after dorsal column lesion in the rat demonstrated that NG2 is highly upregulated and is a major CSPG species. Immunocytochemical analysis further demonstrated that NG2 expression is upregulated within 24 hr of injury, peaks at 1 week, and remains elevated for at least an additional 7 weeks. NG2 expression results from a multicellular response to injury, including both reactive macrophages and oligodendrocyte progenitors; astrocytes were not identified as a major source of NG2. Immunocytochemical analysis of other CSPG family members 7 d after injury showed moderate upregulation of versican, brevican, and neurocan, and downregulation of phosphacan. Axonal tracing experiments demonstrated dense NG2 labeling adjacent to the forward processes of transected corticospinal tract axons in a spatial profile that could restrict axonal growth. Thus, NG2 is a major component of this putatively inhibitory class of ECM molecules expressed at sites of SCI and may restrict axonal regeneration. </p>

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          Author and article information

          Journal
          The Journal of Neuroscience
          J. Neurosci.
          Society for Neuroscience
          0270-6474
          1529-2401
          April 01 2002
          April 01 2002
          April 01 2002
          April 01 2002
          : 22
          : 7
          : 2792-2803
          Article
          10.1523/JNEUROSCI.22-07-02792.2002
          6758310
          11923444
          cc550f48-35f8-44f5-aef7-db111ac98c19
          © 2002
          History

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