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新纹状体中等棘状神经元中多巴胺受体的协同表达。

Coordinated expression of dopamine receptors in neostriatal medium spiny neurons.

作者信息

Surmeier D J, Song W J, Yan Z

机构信息

Department of Anatomy and Neurobiology, College of Medicine, University of Tennessee, Memphis 38163, USA.

出版信息

J Neurosci. 1996 Oct 15;16(20):6579-91. doi: 10.1523/JNEUROSCI.16-20-06579.1996.

Abstract

In recent years, the distribution of dopamine receptor subtypes among the principal neurons of the neostriatum has been the subject of debate. Conventional anatomical and physiological approaches have yielded starkly different estimates of the extent to which D1 and D2 class dopamine receptors are colocalized. One plausible explanation for the discrepancy is that some dopamine receptors are present in physiologically significant numbers, but the mRNA for these receptors is not detectable with conventional techniques. To test this hypothesis, we examined the expression of DA receptors in individual neostriatal neurons by patch-clamp and RT-PCR techniques. Because of the strong correlation between peptide expression and projection site, medium spiny neurons were divided into three groups on the basis of expression of mRNA for enkephalin (ENK) and substance P (SP). Neurons expressing detectable levels of SP but not ENK had abundant mRNA for the D1a receptor. A subset of these cells (approximately 50%) coexpressed D3 or D4 receptor mRNA. Neurons expressing detectable levels of ENK but not SP had abundant mRNA for D2 receptor isoforms (short and long). A subset (10-25%) of these neurons coexpressed D1a or D1b mRNAs. Neurons coexpressing ENK and SP mRNAs consistently coexpressed D1a and D2 mRNAs in relatively high abundance. Functional analysis of neurons expressing lower abundance mRNAs revealed clear physiological consequences that could be attributed to these receptors. These results suggest that, although colocalization of D1a and D2 receptors is limited, functional D1 and D2 class receptors are colocalized in nearly one-half of all medium spiny projection neurons.

摘要

近年来,多巴胺受体亚型在新纹状体主要神经元中的分布一直是争论的焦点。传统的解剖学和生理学方法对D1类和D2类多巴胺受体共定位程度的估计截然不同。对于这种差异,一种合理的解释是,一些多巴胺受体在生理上具有显著数量,但用传统技术无法检测到这些受体的mRNA。为了验证这一假设,我们采用膜片钳和RT-PCR技术检测了单个新纹状体神经元中多巴胺受体的表达。由于肽表达与投射位点之间存在很强的相关性,中等棘状神经元根据脑啡肽(ENK)和P物质(SP)的mRNA表达被分为三组。表达可检测水平的SP但不表达ENK的神经元具有丰富的D1a受体mRNA。这些细胞中的一部分(约50%)共表达D3或D4受体mRNA。表达可检测水平的ENK但不表达SP的神经元具有丰富的D2受体亚型(短型和长型)mRNA。这些神经元中的一部分(10-25%)共表达D1a或D1b mRNA。共表达ENK和SP mRNA的神经元始终以相对较高的丰度共表达D1a和D2 mRNA。对表达较低丰度mRNA的神经元进行功能分析,发现了可归因于这些受体的明显生理后果。这些结果表明,虽然D1a和D2受体的共定位有限,但功能性D1类和D2类受体在几乎一半的中等棘状投射神经元中共定位。

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