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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Entorhinal cortex lesion in adult rats induces the expression of the neuronal chondroitin sulfate proteoglycan neurocan in reactive astrocytes.
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Entorhinal cortex lesion in adult rats induces the expression of the neuronal chondroitin sulfate proteoglycan neurocan in reactive astrocytes.

机译:成年大鼠的内嗅皮质损伤诱导神经元硫酸软骨素蛋白聚糖神经罐在反应性星形胶质细胞中的表达。

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The chondroitin sulfate proteoglycan neurocan is a major component of brain extracellular matrix during development. Neurocan is primarily synthesized by neurons and has the ability to interact with cell adhesion molecules involved in the regulation of cell migration and axonal growth. Within the first weeks postnatally, neurocan expression is strongly downregulated. To test whether neurocan is reexpressed in areas of axonal growth (sprouting) after brain injury, the time course of neurocan expression was analyzed in the denervated fascia dentata of the rat after entorhinal cortex lesion (12 hr; 1, 2, 4, and 10 d; 2 and 4 weeks; and 6 months after lesion). In the denervated zone, immunohistochemistry revealed neurocan-positive astrocytes by 2 d after lesion and a diffuse labeling of the extracellular matrix at all later time points. Electron microscopy confirmed the deposition of neurocan in the extracellular matrix compartment. In situ hybridization demonstrated a strong upregulation of neurocan mRNA within the denervated outer molecular layer 1 and 4 d after lesion. The combination of in situ hybridization with immunohistochemistry for glial fibrillary acidic protein demonstrated that the neurocan mRNA-expressing cells are astrocytes. These data demonstrate that neurocan is reexpressed in the injured brain. In contrast to the situation during development, astrocytes, but not neurons, express neurocan and enrich the extracellular matrix with this molecule. Similar to the situation during development, neurocan is expressed in an area of active axon growth, and it is suggested that neurocan acts to maintain the boundaries of the denervated fascia dentata after entorhinal cortex lesion.
机译:硫酸软骨素蛋白聚糖神经罐是发育过程中脑细胞外基质的主要成分。 Neurocan主要由神经元合成,并具有与参与细胞迁移和轴突生长调节的细胞粘附分子相互作用的能力。在出生后的最初几周内,神经罐的表达强烈下调。为了测试在脑损伤后轴突生长(发芽)区域神经元是否重新表达,分析了内嗅皮质病变(12小时; 1、2、4和10小时)在大鼠失神经筋膜齿状牙本质中神经元表达的时程。 d; 2和4周;以及病变后6个月)。在神经支配区,免疫组化显示病变后2 d神经元阳性星形胶质细胞,并在所有随后的时间点弥漫性标记细胞外基质。电子显微镜检查证实神经罐在细胞外基质区室中的沉积。原位杂交显示在病变后1和4 d失神经外分子层内神经元mRNA的强烈上调。胶质纤维酸性蛋白的原位杂交与免疫组织化学的结合表明神经元mRNA表达细胞是星形胶质细胞。这些数据表明神经cancan在受伤的大脑中重新表达。与发育过程中的情况相反,星形胶质细胞(而不是神经元)表达神经罐并使该分子富集细胞外基质。与发育过程中的情况类似,神经胶质细胞在活跃的轴突生长区域表达,提示神经胶质细胞在内膜皮质病变后可维持失神经的齿状筋膜的边界。

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