Mellon Synthia H, Gong Wenhui, Schonemann Marcus D
Department of Obstetrics, Gynecology and Reproductive Sciences, The Center for Reproductive Sciences, University of California, San Francisco, CA 94143, USA.
Brain Res Rev. 2008 Mar;57(2):410-20. doi: 10.1016/j.brainresrev.2007.05.012. Epub 2007 Jun 12.
The functions for neurosteroids during development and in response to nervous system injury are beginning to be identified. We focused on a mouse model in which we believed neurosteroid production would be altered, and which had a neurodegenerative phenotype. Niemann-Pick Type-C (NP-C) is an autosomal recessive neurodegenerative disease caused by mutations in NPC1 (95%) or NPC2 (5%), resulting in lysosomal accumulation of unesterified cholesterol and glycolipids. The NIH mouse model of NP-C has a mutation in the NPC1 gene, and exhibits several pathological features of the most severe NP-C patients. How lysosomal storage and trafficking defects lead to neurodegeneration is unknown. We found that these mice had normal neurosteroidogenic enzyme activity during development, but lost this activity in the early neonatal period, prior to onset of neurological symptoms. Neurons that expressed P450scc, 3beta HSD, as well as those that expressed 3alpha HSD and 5alpha reductase were lost in adult NP-C brains, resulting in diminished concentrations of allopregnanolone. We treated NP-C mice with allopregnanolone and found that a single dose in the neonatal period resulted in a doubling of life span, substantial delay in onset of neurological symptoms, survival of cerebellar Purkinje and granule cell neurons, and reduction in cholesterol and ganglioside accumulation. The mechanism by which allopregnanolone elicited these effects is unknown. Our in vitro studies showed that Purkinje cell survival promoted by allopregnanolone was lost by treatment with bicuculline, suggesting GABA(A) receptors may play a role. We treated NP-C mice with a synthetic GABA(A) neurosteroid, ganaxolone (3alpha-hydroxy-3beta-methyl-5alpha-pregnan-20-one). Ganaxolone treatment of NP-C mice produced beneficial neurological effects, but these effects were not as robust as those obtained using allopregnanolone. Thus, allopregnanolone may elicit its effects through GABA(A) receptors and through other mechanisms. Additional studies also suggest that allopregnanolone may elicit its effects through pregnane-X-receptors (PXR). Our data suggest that mouse models of neurodegeneration may be beneficial in establishing both physiologic and pharmacologic actions of neurosteroids. These animal models further establish the wide range of functions of these compounds, which may ultimately be useful for treatment of human diseases.
神经甾体在发育过程中以及对神经系统损伤的反应中的功能正开始被确定。我们聚焦于一种小鼠模型,我们认为该模型中神经甾体的产生会发生改变,且具有神经退行性表型。尼曼-匹克C型(NP-C)病是一种常染色体隐性神经退行性疾病,由NPC1(95%)或NPC2(5%)基因的突变引起,导致未酯化胆固醇和糖脂在溶酶体中蓄积。NP-C的美国国立卫生研究院小鼠模型在NPC1基因中有一个突变,并表现出最严重NP-C患者的几种病理特征。溶酶体储存和运输缺陷如何导致神经退行性变尚不清楚。我们发现这些小鼠在发育过程中神经甾体生成酶活性正常,但在新生儿早期,即在神经症状出现之前就失去了这种活性。在成年NP-C小鼠大脑中,表达P450scc、3β-HSD的神经元,以及表达3α-HSD和5α-还原酶的神经元都减少了,导致别孕烯醇酮浓度降低。我们用别孕烯醇酮治疗NP-C小鼠,发现新生儿期单次给药可使寿命延长一倍,神经症状出现时间大幅延迟,小脑浦肯野细胞和颗粒细胞神经元存活,胆固醇和神经节苷脂蓄积减少。别孕烯醇酮产生这些效应的机制尚不清楚。我们的体外研究表明,用荷包牡丹碱处理后,别孕烯醇酮促进的浦肯野细胞存活消失了,这表明GABA(A)受体可能起作用。我们用一种合成的GABA(A)神经甾体加奈索酮(3α-羟基-3β-甲基-5α-孕烷-20-酮)治疗NP-C小鼠。加奈索酮治疗NP-C小鼠产生了有益的神经学效应,但这些效应不如使用别孕烯醇酮时那么显著。因此,别孕烯醇酮可能通过GABA(A)受体以及其他机制发挥其作用。其他研究还表明,别孕烯醇酮可能通过孕烷X受体(PXR)发挥其作用。我们的数据表明,神经退行性变的小鼠模型可能有助于确定神经甾体的生理和药理作用。这些动物模型进一步证实了这些化合物的广泛功能,这最终可能对人类疾病的治疗有用。
