神经甾体雄酮和表雄酮对映体的抗惊厥效力超过了天然形式的效力。
Anticonvulsant potencies of the enantiomers of the neurosteroids androsterone and etiocholanolone exceed those of the natural forms.
作者信息
Zolkowska Dorota, Dhir Ashish, Krishnan Kathiresan, Covey Douglas F, Rogawski Michael A
机构信息
Department of Neurology, University of California, Davis School of Medicine, Sacramento, CA, 20817, USA.
出版信息
Psychopharmacology (Berl). 2014 Sep;231(17):3325-32. doi: 10.1007/s00213-014-3546-x. Epub 2014 Apr 5.
RATIONALE
Androsterone [(3α,5α)-3-hydroxyandrostan-17-one; 5α,3α-A] and its 5β-epimer etiocholanolone [(3α,5β)-3-hydroxyandrostan-17-one; 5β,3α-A)], the major excreted metabolites of testosterone, are neurosteroid positive modulators of GABAA receptors. Such neurosteroids typically show enantioselectivity in which the natural form is more potent than the corresponding unnatural enantiomer. For 5α,3α-A and 5β,3α-A, the unnatural enantiomers are more potent at GABAA receptors than the natural forms.
OBJECTIVES
The aim of this study was to compare the anticonvulsant potencies and time courses of 5α,3α-A and 5β,3α-A with their enantiomers in mouse seizure models.
METHODS
Steroids were administered intraperitoneally to male NIH Swiss mice 15 min (or up to 6 h in time course experiments) prior to administration of an electrical stimulus in the 6-Hz or maximal electroshock (MES) seizure tests or the convulsant pentylenetetrazol (PTZ).
RESULTS
In the 6-Hz test, the ED50 values of ent-5α,3α-A was 5.0 mg/kg whereas the value for 5α,3α-A was 12.1 mg/kg; the corresponding values in the PTZ seizure test were 22.8 and 51.8 mg/kg. Neurosteroid GABAA receptor-positive allosteric modulators are generally weak in the MES seizure test and this was confirmed in the present study. However, the atypical relative potency relationship was maintained with ED50 values of 140 and 223 mg/kg for ent-5α,3α-A and 5α,3α-A, respectively. Similar relationships were obtained for the 5β-isomers, except that the enantioselectivity was accentuated. In the 6-Hz and PTZ tests, the ED50 values of ent-5β,3α-A were 11.8 and 20.4 mg/kg whereas the values for 5β,3α-A were 57.6 and 109.1 mg/kg. Protective activity in the 6-Hz test of ent-5α,3α-A persisted for somewhat longer (5 h) than for 5α,3α-A (4 h); protection by ent-5β,3α-A also persisted longer (3 h) than for 5β,3α-A (2 h).
CONCLUSIONS
The unnatural enantiomers of 17-keto androgen class neurosteroids have greater in vivo potency and a longer duration of action than their natural counterparts. The more prolonged duration of action of the unnatural enantiomers could reflect reduced susceptibility to metabolism. Unnatural enantiomers of androgen class neurosteroids could have therapeutic utility and may provide advantages over the corresponding natural isomers due to enhanced potency and improved pharmacokinetic characteristics.
原理
雄酮[(3α,5α)-3-羟基雄甾烷-17-酮;5α,3α-A]及其5β-差向异构体本胆烷醇酮[(3α,5β)-3-羟基雄甾烷-17-酮;5β,3α-A]是睾酮的主要排泄代谢产物,是GABAA受体的神经甾体阳性调节剂。这类神经甾体通常表现出对映选择性,其中天然形式比相应的非天然对映体更有效。对于5α,3α-A和5β,3α-A,非天然对映体在GABAA受体上比天然形式更有效。
目的
本研究的目的是在小鼠癫痫模型中比较5α,3α-A和5β,3α-A及其对映体的抗惊厥效力和作用时间过程。
方法
在6赫兹或最大电休克(MES)癫痫试验或惊厥性戊四氮(PTZ)中给予电刺激前15分钟(或在时间过程实验中长达6小时),将类固醇腹腔注射给雄性NIH瑞士小鼠。
结果
在6赫兹试验中,对映体-5α,3α-A的半数有效剂量(ED50)值为5.0毫克/千克,而5α,3α-A的值为12.1毫克/千克;在PTZ癫痫试验中的相应值分别为22.8和51.8毫克/千克。神经甾体GABAA受体阳性变构调节剂在MES癫痫试验中通常较弱,本研究证实了这一点。然而,非天然对映体-5α,3α-A和5α,3α-A的ED50值分别为140和223毫克/千克,维持了非典型的相对效力关系。5β-异构体也获得了类似的关系,只是对映选择性更加明显。在6赫兹和PTZ试验中,对映体-5β,3α-A的ED50值分别为11.8和20.4毫克/千克,而5β,3α-A的值分别为57.6和109.1毫克/千克。对映体-5α,3α-A在6赫兹试验中的保护活性持续时间(约5小时)比5α,3α-A(约4小时)稍长;对映体-5β,3α-A的保护作用也比对映体-5β,3α-A(约2小时)持续时间更长(约3小时)。
结论
17-酮雄激素类神经甾体的非天然对映体在体内比其天然对应物具有更大的效力和更长的作用持续时间。非天然对映体作用持续时间延长可能反映出对代谢的敏感性降低。雄激素类神经甾体的非天然对映体可能具有治疗用途,并且由于效力增强和药代动力学特性改善,可能比相应的天然异构体具有优势。
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