Strömberg Jessica, Lundgren Per, Taube Magdalena, Bäckström Torbjörn, Wang Mingde, Haage David
Department of Clinical Science, Umeå Neurosteroid Research Center, Umeå University, Norrlands University Hospital, Umeå, Sweden.
Eur J Pharmacol. 2009 Mar 1;605(1-3):78-86. doi: 10.1016/j.ejphar.2008.12.038. Epub 2009 Jan 10.
The endogenous progesterone metabolite allopregnanolone has a number of properties including anesthetic, sedative, antiepileptic, anxiolytic, impaired memory function and negative mood symptoms. Allopregnanolone is a potent positive GABA(A) receptor function modulators. In contrast, 3beta-hydroxy-steroids (3beta-steroids) usually modulate the GABA(A) receptor negatively. They have attracted some interest for their possible use as therapeutic agents that could counteract the negative symptoms induced by allopregnanolone. Two hypotheses for the action of 3beta-steroids have been proposed: 1) 3beta-steroids act in a similar way to pregnenolone sulphate, which non-competitively reduces GABA(A) receptor activity. 2) 3beta-steroids specifically antagonize the effect of allopregnanolone. We have therefore tried to clarify this issue by comparing the effect of pregnenolone sulphate and 5beta-pregnane-3beta, 20(R)-diol on the GABA-evoked currents by the patch clamp technique on neurons from the medial preoptic nucleus. Both pregnenolone sulphate and 5beta-pregnane-3beta, 20(R)-diol increase the desensitization rate of the current response evoked by a 2 s GABA application. However, their effects on other parameters of the GABA evoked currents differed in degree and sometimes even in direction. The actions of pregnenolone sulphate and 5beta-pregnane-3beta, 20(R)-diol were not altered in the presence of allopregnanolone, which indicates that they do not directly interact with allopregnanolone. In addition, when 5beta-pregnane-3beta, 20(R)-diol was tested on spontaneous inhibitory postsynaptic currents (sIPSCs), it dramatically reduced the allopregnanolone-induced prolongation of the decay time constant but it had no effect on the decay under control conditions. In conclusion, the effect of 5beta-pregnane-3beta, 20(R)-diol on GABA-evoked currents is different to that of pregnenolone sulphate in medial preoptic nucleus neurons.
内源性孕酮代谢产物别孕烯醇酮具有多种特性,包括麻醉、镇静、抗癫痫、抗焦虑、损害记忆功能以及产生负面情绪症状。别孕烯醇酮是一种强效的GABA(A)受体功能正向调节剂。相比之下,3β-羟基类固醇(3β-类固醇)通常对GABA(A)受体起负向调节作用。它们因其可能作为抵消别孕烯醇酮诱导的负面症状的治疗药物而引起了一些关注。关于3β-类固醇的作用提出了两种假说:1)3β-类固醇的作用方式与硫酸孕烯醇酮相似,后者非竞争性地降低GABA(A)受体活性。2)3β-类固醇特异性拮抗别孕烯醇酮的作用。因此,我们试图通过膜片钳技术比较硫酸孕烯醇酮和5β-孕烷-3β,20(R)-二醇对内侧视前核神经元GABA诱发电流的影响来阐明这个问题。硫酸孕烯醇酮和5β-孕烷-3β,20(R)-二醇均增加了2秒GABA应用诱发的电流反应的脱敏率。然而,它们对GABA诱发电流的其他参数的影响在程度上有所不同,有时甚至方向也不同。在存在别孕烯醇酮的情况下,硫酸孕烯醇酮和5β-孕烷-3β,20(R)-二醇的作用未改变,这表明它们不与别孕烯醇酮直接相互作用。此外,当对5β-孕烷-3β,20(R)-二醇进行自发性抑制性突触后电流(sIPSCs)测试时,它显著降低了别孕烯醇酮诱导的衰减时间常数延长,但在对照条件下对衰减没有影响。总之,5β-孕烷-3β,20(R)-二醇对内侧视前核神经元GABA诱发电流的影响与硫酸孕烯醇酮不同。
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