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黑质纹状体多巴胺系统的概念史。

Conceptual history of the nigrostriatal dopamine system.

作者信息

Hattori T

机构信息

Department of Anatomy and Cell Biology, University of Toronto, Ontario, Canada.

出版信息

Neurosci Res. 1993 May;16(4):239-62. doi: 10.1016/0168-0102(93)90035-o.

DOI:10.1016/0168-0102(93)90035-o
PMID:8394552
Abstract

The history of the nigrostriatal dopamine system may provide a prime example of the two faces of scientific development. First, a given concept is replaced by another simply as a result of methodologies being improved, and second, successive technical improvements make seemingly settled controversies even more complicated and disputable. The nigrostriatal pathway, which had been unrecognizable with Nauta's silver impregnation method, became apparent by use of the more sensitive silver impregnation method of Fink-Heimer. The sensitivity of the latter method, however, was still insufficient to reveal the whole extent of another ascending dopamine system, the mesocortical dopamine system, until its existence was established through the application of glyoxylic acid fluorescent histochemistry. Electron microscopic analysis of nigrostriatal dopamine synapses in properly fixed tissue was initiated by the demonstration of dark type terminal degeneration, which was induced by either electrolytic lesions or chemical destruction with a specific toxin (6-hydroxydopamine) of the substantia nigra and medial forebrain bundle. The degenerating terminal boutons, thus produced, invariably formed postsynaptic membrane specializations of asymmetric type. However, the asymmetric nature of the synaptic morphology, although later confirmed by the combined study of chemical lesions and autoradiographic anterograde tracing, was seriously challenged with the introduction of electron microscopic immunohistochemistry. The latter method has consistently revealed that symmetric en passant synapses or axonal varicosities with no synaptic membrane specializations are the only tissue compartments immunoreactive to antibodies against dopamine and its synthetic enzyme tyrosine hydroxylase. In view of the fact that more than 95% of the nigrostriatal projection neurons are dopaminergic, it is difficult to satisfactorily interpret all the available and seemingly paradoxical fine structural data. In this context, a novel concept has emerged in the process of eliminating all the possible alternative interpretations. The concept is that single nigrostriatal neurons form two chemically distinct types of synapses, one dopaminergic symmetric en passant bouton and another non-dopaminergic (still chemically unclassified) asymmetric terminal bouton. If the concept is a valid one, it contradicts Dale's long standing principle, as defined by Eccles: at all the axonal branches of a neuron there is liberation of the same transmitter substance or substances. Furthermore, a certain population of substantia nigra pars reticulata neurons has recently been recognized to be immunoreactive to both dopamine synthetic tyrosine hydroxylase and GABA synthetic glutamate decarboxylase. These single neurons send projections to both the striatum and superior colliculus by way of axon collaterals.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

黑质纹状体多巴胺系统的历史或许能为科学发展的两面性提供一个典型例子。首先,一个既定概念仅仅由于方法学的改进而被另一个概念所取代;其次,连续的技术进步使看似已经解决的争议变得更加复杂且富有争议性。用瑙塔的银浸染法无法辨认的黑质纹状体通路,通过使用更灵敏的芬克 - 海默银浸染法变得清晰可见。然而,后一种方法的灵敏度仍不足以揭示另一个上行多巴胺系统——中脑皮质多巴胺系统的全貌,直到通过应用乙醛酸荧光组织化学法确定了它的存在。对适当固定组织中的黑质纹状体多巴胺突触进行电子显微镜分析,始于对暗型终末变性的证实,这种变性是由电解损伤或用黑质和内侧前脑束的特定毒素(6 - 羟基多巴胺)进行化学破坏所诱导的。由此产生的变性终末小体总是形成不对称型的突触后膜特化结构。然而,突触形态的不对称性质,尽管后来通过化学损伤和放射自显影顺行追踪的联合研究得到了证实,但随着电子显微镜免疫组织化学的引入受到了严重挑战。后一种方法一直表明,对称的旁突触或没有突触膜特化的轴突膨体是唯一对针对多巴胺及其合成酶酪氨酸羟化酶的抗体有免疫反应的组织区室。鉴于超过95%的黑质纹状体投射神经元是多巴胺能的,很难令人满意地解释所有现有的且看似矛盾的精细结构数据。在这种背景下,在排除所有可能的其他解释的过程中出现了一个新的概念。这个概念是单个黑质纹状体神经元形成两种化学性质不同的突触类型,一种是多巴胺能对称旁小体,另一种是非多巴胺能(化学性质仍未分类)不对称终末小体。如果这个概念是有效的,那么它就与戴尔长期以来的原则相矛盾,戴尔的原则由埃克尔斯定义为:在一个神经元的所有轴突分支中释放的是相同的一种或多种递质。此外,最近发现黑质网状部的某些神经元群体对多巴胺合成酶酪氨酸羟化酶和GABA合成酶谷氨酸脱羧酶都有免疫反应。这些单个神经元通过轴突侧支向纹状体和上丘都发出投射。(摘要截取自400字)

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