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大鼠前扣带回皮质(24区)多巴胺能神经支配的产后个体发生。免疫细胞化学和儿茶酚胺荧光组织化学分析。

Postnatal ontogenesis of the dopaminergic innervation in the rat anterior cingulate cortex (area 24). Immunocytochemical and catecholamine fluorescence histochemical analysis.

作者信息

Berger B, Verney C, Febvret A, Vigny A, Helle K B

出版信息

Brain Res. 1985 Jul;353(1):31-47. doi: 10.1016/0165-3806(85)90021-5.

Abstract

The postnatal development of the dopaminergic input to the rat anterior cingulate cortex (area 24) was followed using anti-tyrosine hydroxylase immunocytochemistry and catecholamine fluorescence histochemistry in control and noradrenaline-depleted rats. Noradrenaline depletion in the cerebral cortex was obtained by peripheral injections of 6-hydroxydopamine (6-OHDA) at birth or N-2-chloroethyl-N-ethyl-2-bromobenzylamine (DSP4) at various postnatal ages and controlled by the absence of dopamine-beta-hydroxylase-labelled axons. The superficial and deep components of the anterior cingulate dopaminergic field developed at a different rate in control as well as lesioned rats. The deep supragenual dopaminergic field was already present at birth like the dopaminergic innervation of the prefrontal cortex area 32. In the superficial field, the molecular layer was reached first from postnatal day 3 (P3) on by positive axons running through the anterior hippocampal continuation and from P5-P6 on by another dopaminergic contingent coming through the deep dopaminergic field and giving off collaterals for layer III. The adult distribution pattern and striking varicose aspect were not reached until P21-P30 and a further increased density was observed until P60. The superficial cingulate dopaminergic field extended into the pregenual part of area 24b. The innervation of the superficial and deep layers of the rat anterior cingulate cortex by two distinct dopaminergic subpopulations, one of them closely related to that of prefrontal cortex area 32, could be compared with other laminar differences. The important functional implications of these data are further discussed.

摘要

利用抗酪氨酸羟化酶免疫细胞化学和儿茶酚胺荧光组织化学方法,对正常大鼠和去甲肾上腺素耗竭大鼠中,多巴胺能神经纤维向大鼠前扣带回皮质(24区)的产后发育进行了追踪研究。通过在出生时外周注射6-羟基多巴胺(6-OHDA)或在不同产后年龄注射N-2-氯乙基-N-乙基-2-溴苄胺(DSP4)来实现大脑皮质去甲肾上腺素的耗竭,并通过缺乏多巴胺-β-羟化酶标记轴突来进行控制。在正常大鼠和损伤大鼠中,前扣带回多巴胺能区域的浅层和深层成分发育速度不同。出生时就已存在深层上膝多巴胺能区域,就像前额叶皮质32区的多巴胺能神经支配一样。在浅层区域,从出生后第3天(P3)开始,阳性轴突首先穿过前海马延续部到达分子层,从P5 - P6开始,另一个多巴胺能群体通过深层多巴胺能区域进入并发出侧支到III层。直到P21 - P30才达到成年分布模式和显著的曲张外观,并且在P60之前观察到密度进一步增加。浅层扣带回多巴胺能区域延伸到24b区的膝前部分。大鼠前扣带回皮质浅层和深层由两个不同的多巴胺能亚群支配,其中一个与前额叶皮质32区的关系密切,这可以与其他层状差异进行比较。这些数据的重要功能意义将进一步讨论。

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