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Comparison of the anticonvulsant activity of organic mono- and di-cations and their potential to inhibit NMDA and AMPA glutamate receptors

机译:比较有机单阳离子和双阳离子的抗惊厥活性及其抑制NMDA和AMPA谷氨酸受体的潜力

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摘要

Effects of mono- and dicationic derivatives of adamantine and phenylcyclohexyl were studied on: (i) open channels of NMDA and AMPA glutamate receptors in the experiments on the isolated rat brain neurones, and (ii) convulsions induced by intraventricular injections of NMDA or kainate in mice. Monocations inhibited the NMDA receptors in vitro and prevented convulsions induced by NMDA in vivo, but failed to affect both the AMPA receptors and kainite-induced convulsions. Dications (IEM-1754 and IEM-1925) revealed both anti-NMDA and anti-AMPA potency in vitro, were highly effective against kainite-induced convulsions and excelled monocations in preventing the NMDA-induced ones. Evidently some steps connected with the AMPA receptor activity are involved in the genesis of the NMDA-induced convulsions. Anticonvulsant potency of IEM-1754 and IEM-1925 is comparable with those of known NMDA receptor inhibitors: memantine and MK-801. The IEM-1754 and IEM-1925 show no side effects. An incomplete correspondence between the activity in vitro and in vivo found studying some derivatives, may be due to peculiarities of their pharmacokinetics.
机译:研究了金刚烷和苯基环己基的单价和单价衍生物的作用:(i)在离体大鼠脑神经元的实验中,NMDA和AMPA谷氨酸受体的开放通道;(ii)脑室内注射NMDA或海藻酸盐诱导的惊厥老鼠。单阳离子在体外抑制NMDA受体,并在体内阻止由NMDA引起的惊厥,但不能同时影响AMPA受体和贝氏体引起的惊厥。阳离子(IEM-1754和IEM-1925)在体外显示出抗NMDA和抗AMPA的功效,对抵抗凯因石引起的惊厥非常有效,并且在防止NMDA引起的惊厥方面表现出优异的单阳离子。显然,与AMPA受体活性有关的某些步骤与NMDA诱发的惊厥的发生有关。 IEM-1754和IEM-1925的抗惊厥作用与已知的NMDA受体抑制剂美金刚和MK-801相当。 IEM-1754和IEM-1925没有副作用。研究某些衍生物时发现的体内和体外活性之间的不完全对应可能是由于它们的药代动力学特性所致。

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