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点燃过程中血管加压素mRNA的变化:点燃部位和阶段的影响。

Vasopressin mRNA changes during kindling: the effects of kindling site and stage.

作者信息

Greenwood R S, Abdou A, Meeker R B, Hayward J N

机构信息

Department of Neurology and Pediatrics, University of North Carolina School of Medicine, Chapel Hill 27599.

出版信息

Brain Res Mol Brain Res. 1994 Oct;26(1-2):286-92. doi: 10.1016/0169-328x(94)90101-5.

Abstract

Because of the many anatomical and functional links to the limbic system, the neuroendocrine system is often affected by limbic disturbances. Limbic seizures in humans and animals alter neuroendocrine function and hormone levels. We have shown that in an animal model for partial seizures, the amygdala kindled rat, plasma vasopressin levels are elevated and a sustained increase in vasopressin (VP) mRNA follows stage 5 kindled seizures. In the present experiments we sought to determine when during the course of amygdala kindling the VP mRNA increase occurs and whether specific anatomical pathways mediate this increase. Animals kindled to early seizure stages (stages 1, 2 or 3) had no consistent increase in VP mRNA in the supraoptic nucleus (SON) while animals kindled to generalized seizures, stages 4 or 5, invariably had increased VP mRNA relative to controls. Electrical kindling to stage 5 seizures from two other brain sites, the dorsal hippocampus and the anterior olfactory nucleus, consistently resulted in a significant increase in VP mRNA one week after completing kindling. In all experiments the increase in VP mRNA in the SON showed no differences related to the side or proximity of the electrodes used for kindling. Measures of water balance did not change following kindling. These results indicate that kindled seizure generalization is a prerequisite for the long-term increase in VP mRNA. Furthermore, the VP mRNA increase appears to involve polysynaptic pathways accessible from different limbic kindling sites. These studies support the hypothesis that changes in mRNA regulation may contribute to the neuroendocrine pathophysiology accompanying limbic seizures.

摘要

由于与边缘系统存在诸多解剖学和功能上的联系,神经内分泌系统常常受到边缘系统紊乱的影响。人类和动物的边缘性癫痫发作会改变神经内分泌功能和激素水平。我们已经表明,在部分性癫痫发作的动物模型——杏仁核点燃大鼠中,血浆血管加压素水平会升高,并且在5期点燃癫痫发作后,血管加压素(VP)mRNA会持续增加。在本实验中,我们试图确定在杏仁核点燃过程中VP mRNA增加发生的时间,以及是否有特定的解剖学通路介导这种增加。点燃至癫痫发作早期阶段(1、2或3期)的动物,视上核(SON)中的VP mRNA没有持续增加,而点燃至全身性癫痫发作阶段(4或5期)的动物,相对于对照组,其VP mRNA总是增加。从另外两个脑区,即背侧海马体和前嗅核,电刺激点燃至5期癫痫发作,在完成点燃一周后,始终导致VP mRNA显著增加。在所有实验中,SON中VP mRNA的增加与用于点燃的电极的一侧或距离无关。点燃后水平衡指标没有变化。这些结果表明,点燃癫痫发作的全身性扩散是VP mRNA长期增加的先决条件。此外,VP mRNA的增加似乎涉及从不同边缘性点燃部位可及的多突触通路。这些研究支持这样一种假说,即mRNA调节的变化可能促成伴随边缘性癫痫发作的神经内分泌病理生理学改变。

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