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神经元特异性烯醇化酶作为神经元再生和神经再支配的指标。

Neuron-specific enolase as an index of neuronal regeneration and reinnervation.

作者信息

Kirino T, Brightman M W, Oertel W H, Schmechel D E, Marangos P J

出版信息

J Neurosci. 1983 May;3(5):915-23. doi: 10.1523/JNEUROSCI.03-05-00915.1983.

Abstract

Neuron-specific enolase (NSE) is a glycolytic isoenzyme which is located in central and peripheral neurons and neuroendocrine cells. Another enolase isoenzyme, non-neuronal enolase (NNE), occurs in glial cells. The purpose of this study was to follow any changes in NSE and/or NNE in cranial motor neurons after separation of their cell bodies from their axon terminals. One hypoglossal nerve in the rat and the cynomolgus monkey was thus crushed or cut and, after a given period, the brains were perfusion fixed. Immunocytochemistry, using anti-rat NSE and NNE or anti-human NSE and NNE, was performed on Vibratome-sectioned specimens of the hypoglossal nuclei. In the rat, NSE immunostaining decreased in the affected neurons 2 to 10 days following axonal injury. The change was greatest on the 10th day. Twenty days following nerve crush. NSE staining began to recover on the operated side and by the 45th day had returned to normal levels. NSE changes in the monkey were similar to those in the rat. In rats, where the nerve was cut and the proximal stump was translocated to a normally innervated muscle to inhibit re-formation of synaptic contacts, the NSE remained low for 60 days after nerve injury. As NSE levels fell during degeneration, there was a slight increase in NNE in some of the monkey specimens but not in others; the NNE alterations were, therefore, equivocal. The results demonstrate that the content of NSE in neurons serves as a molecular marker of axon injury, regeneration, and target reinnervation.

摘要

神经元特异性烯醇化酶(NSE)是一种糖酵解同工酶,位于中枢和外周神经元以及神经内分泌细胞中。另一种烯醇化酶同工酶,非神经元烯醇化酶(NNE),存在于神经胶质细胞中。本研究的目的是追踪颅运动神经元的细胞体与其轴突终末分离后NSE和/或NNE的任何变化。因此,对大鼠和食蟹猴的一条舌下神经进行挤压或切断,在给定时间段后,对大脑进行灌注固定。使用抗大鼠NSE和NNE或抗人NSE和NNE,对舌下神经核的振动切片标本进行免疫细胞化学检测。在大鼠中,轴突损伤后2至10天,受影响神经元中的NSE免疫染色减少。第10天时变化最大。神经挤压后20天,手术侧的NSE染色开始恢复,到第45天时已恢复到正常水平。猴子中的NSE变化与大鼠相似。在大鼠中,切断神经并将近端残端移位到正常支配的肌肉以抑制突触接触的重新形成,神经损伤后60天NSE仍保持低水平。随着变性过程中NSE水平下降,一些猴子标本中的NNE略有增加,但其他标本中没有;因此,NNE的变化不明确。结果表明,神经元中NSE的含量可作为轴突损伤、再生和靶神经再支配的分子标记。

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