Uzunova Veska, Sampson Luther, Uzunov Doncho P
Neuroscience Research, Novartis Institutes for BioMedical Research, Novartis Pharma AG, WSJ-386.3.264002, Basel, Switzerland.
Psychopharmacology (Berl). 2006 Jun;186(3):351-61. doi: 10.1007/s00213-005-0201-6. Epub 2005 Oct 26.
The naturally occurring 3alpha-reduced neurosteroids allopregnanolone and its isomer pregnanolone are among the most potent positive allosteric modulators of gamma-aminobutyric acid type A receptors. They play a critical role in the maintenance of physiological GABAergic tone and display a broad spectrum of neuropsychopharmacological properties. We have reviewed existing evidence implicating the relevance of endogenous 3alpha-reduced neuroactive steroids to depression and to the mechanism of action of antidepressants. A wide range of preclinical and clinical evidence suggesting the antidepressant potential of 3alpha-reduced neuroactive steroids and a possible involvement of a deficiency and a disequilibrium of neuroactive steroid levels in pathomechanisms underlying the etiology of major depressive disorder have emerged in recent years. Antidepressants elevate 3alpha-reduced neurosteroid levels in rodent brain, and clinically effective antidepressant pharmacotherapy is associated with normalization of plasma and cerebrospinal fluid (CSF) concentrations of endogenous neuroactive steroids in depressed patients, unveiling a possible contribution of neuroactive steroids to the mechanism of action of antidepressants. In contrast, recent studies using nonpharmacological antidepressant therapy suggest that changes in plasma neuroactive steroid levels may not be a general mandatory component of clinically effective antidepressant treatment per se, but may reflect distinct properties of pharmacotherapy only. While preclinical studies offer convincing evidence in support of an antidepressant-like effect of 3alpha-reduced neuroactive steroids in rodent models of depression, current clinical investigations are inconclusive of an involvement of neuroactive steroid deficiency in the pathophysiology of depression. Moreover, clinical evidence is merely suggestive of a role of neuroactive steroids in the mechanism of action of clinically effective antidepressant therapy. Additional clinical studies evaluating the impact of successful pharmacological and nonpharmacological antidepressant therapies on changes in neuroactive steroid levels in both plasma and CSF samples of the same patients are necessary in order to more accurately address the relevance of 3alpha-reduced neuroactive steroids to major depressive disorder. Finally, proof-of-concept studies with drugs that are known to selectively elevate brain neurosteroid levels may offer a direct assessment of an involvement of neurosteroids in the treatment of depressive symptomatology.
天然存在的3α-还原神经甾体别孕烯醇酮及其异构体孕烷醇酮是γ-氨基丁酸A型受体最有效的正变构调节剂之一。它们在维持生理性γ-氨基丁酸能张力中起关键作用,并表现出广泛的神经精神药理学特性。我们综述了现有证据,这些证据表明内源性3α-还原神经活性甾体与抑郁症以及抗抑郁药的作用机制相关。近年来,大量临床前和临床证据表明3α-还原神经活性甾体具有抗抑郁潜力,且在重度抑郁症病因的病理机制中,神经活性甾体水平的缺乏和失衡可能发挥作用。抗抑郁药可提高啮齿动物脑中3α-还原神经甾体的水平,临床上有效的抗抑郁药物治疗与抑郁症患者血浆和脑脊液(CSF)中内源性神经活性甾体浓度的正常化相关,这揭示了神经活性甾体可能对抗抑郁药的作用机制有贡献。相比之下,最近使用非药物抗抑郁治疗的研究表明,血浆神经活性甾体水平的变化本身可能不是临床上有效抗抑郁治疗的普遍必需组成部分,而可能仅反映药物治疗的独特特性。虽然临床前研究提供了令人信服的证据,支持3α-还原神经活性甾体在啮齿动物抑郁症模型中具有抗抑郁样作用,但目前的临床研究对于神经活性甾体缺乏是否参与抑郁症的病理生理学尚无定论。此外,临床证据仅提示神经活性甾体在临床上有效抗抑郁治疗的作用机制中发挥作用。为了更准确地探讨3α-还原神经活性甾体与重度抑郁症的相关性,有必要进行更多临床研究,评估成功的药物和非药物抗抑郁治疗对同一患者血浆和脑脊液样本中神经活性甾体水平变化的影响。最后,使用已知能选择性提高脑内神经甾体水平的药物进行概念验证研究,可能会直接评估神经甾体在治疗抑郁症状中的作用。
