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富含神经肌肉接头的肌肉区域神经再生过程中胰岛素样生长因子基因表达的时间依赖性改变。

Time-dependent alteration of insulin-like growth factor gene expression during nerve regeneration in regions of muscle enriched with neuromuscular junctions.

作者信息

Pu S F, Zhuang H X, Marsh D J, Ishii D N

机构信息

Department of Physiology and Department of Biochemistry and Molecular Biology, Colorado State University, Fort Collins, CO 80523, USA.

出版信息

Brain Res Mol Brain Res. 1999 Jan 8;63(2):207-16. doi: 10.1016/s0169-328x(98)00250-2.

Abstract

Insulin-like growth factors (IGFs) increase the rate of motor axon elongation, prevent motoneuron death, and may support the reestablishment of synapses following nerve injury. In situ hybridization was used in the present study to examine the temporal and spatial distribution of IGF gene expression in soleus muscle following sciatic nerve crush in rats. In intact muscle, IGF-II gene expression was generally low, and localized to interstitial cells, possibly fibroblast and Schwann cells. These cells were found in the middle of muscle which is enriched in neuromuscular junctions. IGF-II gene expression, 4-6 days postcrush, was increased in interstitial cells. Thereafter, IGF-II gene expression was also increased in muscle cells or cells closely associated with muscle fibers, such as satellite cells. IGF-II gene expression was increased to a much greater extent in the midregion of muscle enriched in end-plates than in the two ends of muscle, but returned towards normal following the reestablishment of functional synapses. On the other hand, IGF-I gene expression was only slightly increased following nerve crush, and this increase was associated with interstitial, but not muscle cells. These results show that the IGF-I and IGF-II genes are regulated by independent signals and may play separate roles during nerve regeneration. For example, a regional increase in IGF-II gene expression may support preferential nerve terminal sprouting in the middle of muscle enriched in neuromuscular junctions, thereby increasing the probability for the reestablishment of synapses.

摘要

胰岛素样生长因子(IGFs)可提高运动轴突的伸长速率,防止运动神经元死亡,并可能支持神经损伤后突触的重建。在本研究中,采用原位杂交技术检测大鼠坐骨神经挤压伤后比目鱼肌中IGF基因表达的时间和空间分布。在完整肌肉中,IGF-II基因表达普遍较低,且定位于间质细胞,可能是成纤维细胞和雪旺细胞。这些细胞存在于富含神经肌肉接头的肌肉中部。挤压伤后4-6天,间质细胞中IGF-II基因表达增加。此后,肌肉细胞或与肌纤维密切相关的细胞(如卫星细胞)中IGF-II基因表达也增加。与肌肉两端相比,富含终板的肌肉中部IGF-II基因表达增加的程度要大得多,但在功能性突触重建后又恢复到正常水平。另一方面,神经挤压伤后IGF-I基因表达仅略有增加,且这种增加与间质细胞而非肌肉细胞有关。这些结果表明,IGF-I和IGF-II基因受独立信号调控,在神经再生过程中可能发挥不同作用。例如,IGF-II基因表达的区域性增加可能支持富含神经肌肉接头的肌肉中部优先发生神经末梢发芽,从而增加突触重建的可能性。

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