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Effects and mechanism of action of isatin, a MAO inhibitor, on in vivo striatal dopamine release

机译:Isatin,毛泽东抑制剂,体内纹状体多巴胺释放作用的影响及机制

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Isatin is an endogenous indole that inhibits monoamine oxidase (MAO), being more selective for MAO-B than MAO-A isoform. By inhibiting MAO, isatin increases dopamine levels in the brain and, in animal models of Parkinson's disease (PD) isatin is able to prevent dopamine depletion. Contradictorily, some studies indicate that isatin did not increase striatal dopamine levels, although it was able to improve the motor signs in PD model. Given these conflicting data, our aim was to study the effects and neurochemical mechanisms of action of isatin on in vivo dopamine release from rat dorsal striatum using brain microdialysis technique in conscious and freely moving animals. Our results showed that intrastriatal administration of 1, 5 or 10 mM isatin, for 1 h, significantly increased dopamine levels to 355 104%, 700 +/- 72%, and 1241 +/- 146%, when compared with basal values, respectively. The highest concentration of isatin (10 mM) was used to investigate whether the dopamine overflow is due to an exocytotic release or due to a possible action on dopamine transporter (DAT). The removal of Ca++ from medium, administration of TTX (10 mu M), or pretreatment with reserpine (10 mg/kg) significantly decreased by 90%, 83%, and 78%, respectively, the effect of isatin on dopamine levels. The blockade of DAT with nomifensine (50 mu M) did not alter the effect of isatin; and isatin significantly increased the depolarization-evoked release of dopamine. These results suggest that isatin-induced dopamine release depends on vesicular dopamine content, and takes place due to a previous entry of Ca++ and terminal depolarization. (C) 2016 Published by Elsevier Ltd.
机译:Isatin是一种内源性吲哚,其抑制单胺氧化酶(MAO),对于MAO-B的MAO-B更具选择性。通过抑制毛泽,Isatin增加了大脑中的多巴胺水平,并且在帕金森病(Pd)的动物模型中,Isatin能够预防多巴胺耗尽。矛盾地,一些研究表明,Isatin没有增加纹状体多巴胺水平,尽管它能够改善PD模型中的电机标志。鉴于这些冲突的数据,我们的目的是研究在有意识和自由移动的动物中使用脑微透视技术从大鼠背体释放等体内二巴胺释放的isatin释放的效果和神经化学机制。我们的研究结果表明,与基本值相比,1小时,1小时,1小时,1小时,含量为1,5或10毫米isatin,其显着增加至355.104%,700 +/- 72%和1241 +/- 146% 。使用最高浓度的Isatin(10mM)来研究多巴胺溢出是否是由于杂种释放或由于多巴胺转运蛋白(DAT)的可能作用。从培养基中除去Ca ++,施用TTX(10μm),或与血纯度(10mg / kg)的预处理分别显着降低了90%,83%和78%,isatin对多巴胺水平的影响。 Nomifensine(50 mu m)的DAT封锁没有改变Isatin的效果; isatin显着增加了多巴胺的去极化诱发的释放。这些结果表明,Isatin诱导的多巴胺释放取决于囊泡多巴胺含量,并且由于进一步的Ca ++和末端去极化而发生。 (c)2016由elestvier有限公司出版

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