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首页> 外文期刊>Journal of psychiatric research >Accumulated increase in neuropeptide Y and somatostatin gene expression of the rat in response to repeated electroconvulsive stimulation.
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Accumulated increase in neuropeptide Y and somatostatin gene expression of the rat in response to repeated electroconvulsive stimulation.

机译:反复电惊厥刺激大鼠神经肽Y和生长抑素基因表达的累积增加。

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The mechanisms by which electroconvulsive therapy (ECT) causes its antidepressive effect are unknown. Because ECT requires repeated induction of electroconvulsive seizures, adaptive changes in the brain and regulation of gene expression, are likely to be the fundamental basis on which ECT acts. Neuropeptide Y (NPY) gene expression is increased after multiple electroconvulsive stimulations (ECS) and since it also has anticonvulsant and antidepressant properties, it has led to the hypothesis that the beneficial effect of ECT is mediated via its activation of NPY-dependent neurotransmission. We have therefore examined in detail the temporal profile of NPY gene expression, using in situ hybridisation histochemistry in the rat dentate gyrus and piriform cortex - two brain areas centrally involved in seizure regulation. NPY mRNA in both regions was found to increase gradually with the number of ECS, reaching a maximum (550-700%) after approximately 14 ECS where no further increase was achieved by additional ECS. A number of 14 ECS was also shown to exert anticonvulsant activity against kainic acid seizures. In the dentate gyrus, repeated ECS also caused a gradual, but smaller, increase in the expression of somatostatin (SS) - a neuropeptide that is co-localised with NPY and also has anticonvulsant effects. These results shows that NPYergic and, to a lesser extent, SSergic neurotransmission is activated by ECS and support the hypothesis that these neuropeptides could play a central role in the anticonvulsant and antidepressant effect of ECT.
机译:电惊厥疗法(ECT)引起其抗抑郁作用的机制尚不清楚。由于ECT需要反复诱发电痉挛性癫痫发作,因此大脑的适应性变化和基因表达的调节可能是ECT作用的基础。多次电惊厥刺激(ECS)后神经肽Y(NPY)基因表达增加,并且由于它还具有抗惊厥和抗抑郁特性,因此导致了这样一个假设,即ECT的有益作用是通过其激活NPY依赖性神经传递而介导的。因此,我们在大鼠齿状回和梨状皮层中使用了原位杂交组织化学方法,详细研究了NPY基因表达的时间变化。这两个大脑区域主要参与癫痫发作的调节。发现这两个区域中的NPY mRNA随着ECS数量的增加而逐渐增加,在大约14个ECS之后达到最大值(550-700%),而其他ECS则没有进一步增加。还显示了14个ECS对海藻酸癫痫发作具有抗惊厥作用。在齿状回中,重复的ECS也会导致生长抑素(SS)的表达逐渐增加,但增幅较小,这是一种与NPY共同定位并且还具有抗惊厥作用的神经肽。这些结果表明,NPYergic和SSergic的神经传递被ECS激活,并支持这些神经肽可能在ECT的抗惊厥和抗抑郁作用中发挥重要作用的假设。

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