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酪氨酸羟化酶在培养大脑皮层神经元中的表达:中枢神经系统神经元表型可塑性的证据。

Expression of tyrosine hydroxylase in neurons of cultured cerebral cortex: evidence for phenotypic plasticity in neurons of the CNS.

作者信息

Iacovitti L, Lee J, Joh T H, Reis D J

出版信息

J Neurosci. 1987 Apr;7(4):1264-70. doi: 10.1523/JNEUROSCI.07-04-01264.1987.

Abstract

In vivo, neurons of the cerebral cortex of rat embryos did not stain with antibodies to the catecholamine (CA) biosynthetic enzyme tyrosine hydroxylase (TH) even when examined using a highly sensitive technique for radioimmunocytochemistry. However, when embryonic day (E) 13 cortex was grown 1 d in culture, several thousand cells expressed immunoreactive and catalytically active TH. All TH cells simultaneously labeled with the neuronal enzyme, neuronal specific enolase, indicating that the TH was exclusively localized in neurons. Moreover, all TH neurons were postmitotic since they did not incorporate 3H-thymidine. With time in culture, the number of TH cells selectively declined from nearly 3000 cells at 2 d to several cells at 14 d. Similarly, the number of neurons competent to express TH in culture declined with advancing age of the donor embryo. Thus, by E18, very few cortical neurons had the capacity to express TH. We conclude that during a critical period of development, postmitotic cerebral cortical neurons can express catecholamine traits in vitro but not in vivo. Thus, the neurotransmitter phenotype of certain classes of central neurons is not fixed but can be influenced by epigenetic factors found in their environment, thereby providing evidence of phenotypic plasticity in the central nervous system (CNS).

摘要

在体内,即使采用高灵敏度的放射免疫细胞化学技术检测,大鼠胚胎大脑皮质的神经元也不会被针对儿茶酚胺(CA)生物合成酶酪氨酸羟化酶(TH)的抗体染色。然而,当将胚胎第13天(E13)的皮质在培养中生长1天时,数千个细胞表达了具有免疫反应性和催化活性的TH。所有表达TH的细胞同时被神经元酶神经元特异性烯醇化酶标记,这表明TH仅定位于神经元中。此外,所有表达TH的神经元都已完成有丝分裂,因为它们不掺入3H-胸腺嘧啶核苷。随着培养时间的延长,表达TH的细胞数量从第2天的近3000个细胞选择性地减少到第14天的几个细胞。同样,培养中能够表达TH的神经元数量随着供体胚胎年龄的增加而减少。因此,到E18时,很少有皮质神经元具有表达TH的能力。我们得出结论,在发育的关键时期,有丝分裂后的大脑皮质神经元在体外而非体内能够表达儿茶酚胺特性。因此,某些类型的中枢神经元的神经递质表型并非固定不变,而是可受其环境中表观遗传因素的影响,从而为中枢神经系统(CNS)中的表型可塑性提供了证据。

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