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面部和红核脊髓神经元对轴突切断的反应:细胞骨架蛋白和GAP - 43的mRNA表达变化

Response of facial and rubrospinal neurons to axotomy: changes in mRNA expression for cytoskeletal proteins and GAP-43.

作者信息

Tetzlaff W, Alexander S W, Miller F D, Bisby M A

机构信息

Departments of Anatomy, University of Calgary, Alberta, Canada.

出版信息

J Neurosci. 1991 Aug;11(8):2528-44. doi: 10.1523/JNEUROSCI.11-08-02528.1991.

Abstract

Neurons confined within the mammalian CNS usually do not regenerate after axonal injury, while axonal regeneration is the rule in the PNS. It has been hypothesized that this may be related to differences in the microenvironment of the PNS versus CNS and to differences in the neuronal response to injury. In order to test the latter hypothesis, we compared changes in gene expression after axotomy in two populations of neurons: rat facial motoneurons and rat rubrospinal neurons. In situ hybridization with cDNA probes for the medium and light neurofilament protein revealed a reduced mRNA content in both facial and rubrospinal neurons at all times investigated (i.e., 1, 2, and 3 weeks after axotomy). On the other hand, mRNAs for actin and tubulin were increased in both neuronal populations during the first week after axotomy. While this increase was sustained in facial motoneurons for several weeks, total tubulin mRNA and actin mRNA were decreased in rubrospinal neurons at 2 and 3 weeks after axotomy, coincident with their atrophy. The developmentally regulated T alpha 1 tubulin mRNA, which was previously shown to be reexpressed in facial motoneurons after axotomy, was elevated severalfold in axotomized rubrospinal neurons, and increased levels persisted in some rubrospinal neurons as late as 7 weeks after axotomy. Similarly, the developmentally regulated GAP-43 mRNA increased in both axotomized facial and rubrospinal neurons, and increased levels were sustained in some axotomized rubrospinal neurons for at least 7 weeks. The response of rubrospinal neurons to axotomy in the cervical spinal cord is, in the first week, qualitatively similar to the response of facial motoneurons. However, by 2 weeks after axotomy there is a generalized reduction in mRNA levels for all three cytoskeletal proteins that is associated with neuronal atrophy. During this period, mRNA levels for the two specific markers of the growth state, T alpha 1 tubulin and GAP-43, remain elevated. Thus, axotomy of rubrospinal neurons appears to set in motion two independent events. First, an axotomy signal initiates a cell-body reaction similar to that of PNS neurons, including increased mRNA levels for T alpha 1 tubulin and GAP-43. Later, a generalized cellular atrophy and decrease in mRNA levels occur without reversing the specific responses of T alpha 1 and GAP-43 to axotomy. We conclude that the failure of rubrospinal neurons to regenerate is not due to a failure to initiate gene-expression changes characteristic of regenerating peripheral neurons.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

哺乳动物中枢神经系统(CNS)内的神经元在轴突损伤后通常不会再生,而轴突再生在周围神经系统(PNS)中则是常见现象。据推测,这可能与PNS和CNS微环境的差异以及神经元对损伤的反应差异有关。为了验证后一种假设,我们比较了两种神经元群体(大鼠面神经运动神经元和大鼠红核脊髓神经元)轴突切断后基因表达的变化。用中等和轻型神经丝蛋白的cDNA探针进行原位杂交显示,在所有研究时间点(即轴突切断后1、2和3周),面神经和红核脊髓神经元中的mRNA含量均降低。另一方面,在轴突切断后的第一周,两种神经元群体中的肌动蛋白和微管蛋白mRNA均增加。虽然这种增加在面神经运动神经元中持续了数周,但在轴突切断后2周和3周,红核脊髓神经元中的总微管蛋白mRNA和肌动蛋白mRNA减少,这与它们的萎缩相一致。发育调控的Tα1微管蛋白mRNA先前已被证明在轴突切断后的面神经运动神经元中重新表达,在轴突切断的红核脊髓神经元中其水平升高了几倍,并且在一些红核脊髓神经元中,其增加的水平一直持续到轴突切断后7周。同样,发育调控的GAP - 43 mRNA在轴突切断的面神经和红核脊髓神经元中均增加,并且在一些轴突切断的红核脊髓神经元中,增加的水平至少持续了7周。红核脊髓神经元对颈脊髓轴突切断的反应在第一周与面神经运动神经元的反应在性质上相似。然而,在轴突切断后2周,所有三种细胞骨架蛋白的mRNA水平普遍降低,这与神经元萎缩有关。在此期间,生长状态的两种特异性标志物Tα1微管蛋白和GAP - 43的mRNA水平仍然升高。因此,红核脊髓神经元轴突切断似乎引发了两个独立的事件。首先,轴突切断信号引发了类似于PNS神经元的细胞体反应,包括Tα1微管蛋白和GAP - 43的mRNA水平增加。后来,出现了普遍的细胞萎缩和mRNA水平降低,但并没有逆转Tα1和GAP - 43对轴突切断的特异性反应。我们得出结论,红核脊髓神经元不能再生并非由于未能启动再生外周神经元特有的基因表达变化。(摘要截取自400字)

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