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首页> 外文期刊>Experimental Neurology >Improved sciatic nerve regeneration by local thyroid hormone treatment in adult rat is accompanied by increased expression of SCG10.
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Improved sciatic nerve regeneration by local thyroid hormone treatment in adult rat is accompanied by increased expression of SCG10.

机译:成年大鼠通过局部甲状腺激素治疗改善坐骨神经再生,并伴有SCG10表达的增加。

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Thyroid hormone plays an important role in regulating the development and regeneration of the nervous system. Our previous work showed that local administration of triiodothyronine (T3) at the level of transected rat sciatic nerve increased the number and diameter of regenerated axons, but the mechanism underlying the improved regeneration is still unclear. Here, we have investigated the effect of T3 on the expression of SCG10, a regulator of microtubule dynamics in growth cones. After transection of adult rat sciatic nerves, silicone tubes were implanted and filled with T3 or phosphate-buffered solution. At various time points following surgery, the expression of SCG10 protein and mRNA was analyzed. Semi-quantitative Western blot analysis revealed that sciatic nerve transection induced a more than 20-fold upregulation of SCG10 protein in proximal nerve segments at 1 day post-lesion, while at this time point, SCG10 mRNA in dorsal root ganglion neurons was not increased yet. The increase in SCG10 protein and mRNA could be observed over 30 days. Local T3 treatment significantly enhanced the increase in SCG10 protein levels about two-fold in the different segments of transected nerve during the regeneration period. Also SCG10 mRNA levels in lumbar ganglia were enhanced. Immunohistochemical analysis showed that T3 treatment not only increased the number of SCG10 positive axons but also the intensity of their staining. These results suggest that SCG10 is involved in the regulation of regeneration. The stimulating effect of T3 on SCG10 expression could provide a mechanism by which T3 enhances peripheral nerve regeneration.
机译:甲状腺激素在调节神经系统的发育和再生中起重要作用。我们以前的工作表明,在横切大鼠坐骨神经的水平局部施用三碘甲状腺素(T3)可增加再生轴突的数量和直径,但改善再生的基础机制仍不清楚。在这里,我们研究了T3对SCG10表达的影响,SCG10是生长锥中微管动力学的调节剂。成年大鼠坐骨神经横切后,植入硅胶管并填充T3或磷酸盐缓冲液。在手术后的各个时间点,分析SCG10蛋白和mRNA的表达。半定量蛋白质印迹分析显示,在损伤后1天,坐骨神经横断导致近端神经节中SCG10蛋白上调20倍以上,而此时,背根神经节神经元中SCG10 mRNA尚未增加。在30天内可以观察到SCG10蛋白和mRNA的增加。在再生期间,局部T3处理显着增强了横断神经不同节段中SCG10蛋白水平的增加,约为两倍。腰神经节中的SCG10 mRNA水平也增加。免疫组织化学分析表明,T3处理不仅增加了SCG10阳性轴突的数量,而且增加了其染色强度。这些结果表明SCG10参与再生的调节。 T3对SCG10表达的刺激作用可以提供一种机制,通过该机制T3可以增强周围神经的再生。

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