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鹌鹑视前区中芳香化酶活性的直接多巴胺能调控。

A direct dopaminergic control of aromatase activity in the quail preoptic area.

作者信息

Baillien M, Balthazart J

机构信息

Laboratory of Biochemistry, University of Liège, Belgium.

出版信息

J Steroid Biochem Mol Biol. 1997 Sep-Oct;63(1-3):99-113. doi: 10.1016/s0960-0760(97)00080-0.

DOI:10.1016/s0960-0760(97)00080-0
PMID:9449211
Abstract

In the quail preoptic area (POA) anatomical and pharmacological data suggest that catecholamines may be implicated in the control of testosterone (T) aromatization into estrogens. The biochemical mechanism(s) mediating this control of the enzyme activity is (are) however unexplored. The present studies were carried out to investigate whether the catecholamines, dopamine (DA) and norepinephrine (NE) are able to directly affect aromatase activity (AA) measured during in vitro incubations of POA homogenates. AA was quantified in the POA-hypothalamus of adult male Japanese quail by measuring the tritiated water production from [1beta-3H]-androstenedione. Enzyme activity was linear as a function of the incubation time and of the protein content of homogenates. It exhibited a typical Michaelis-Menten kinetics, with an apparent Km of 2.8 nM and a Vmax of 266.6 fmol h(-1) mg wet weight(-1). AA was then measured at a substrate concentration of 25 nM in the presence of catecholamines and some of their receptor agonists or antagonists, at two concentrations, 10(-3) and 10(-6) M. Norepinephrine and prazosin (alpha1-adrenergic antagonist) had no or very limited effects on AA at both concentrations. In contrast, DA and some D1 and/or D2 receptor agonists (apomorphine[D1/D2], SKF-38393 [D1] and RU-24213 [D2]) depressed AA by 40 to 70% at the 10(-3) M concentration. One D2 receptor antagonist also produced a major inhibition of AA (sulpiride) while other antagonists either had no significant effect or only produced moderate decreases in enzyme activity (SCH-23390 [D1], spiperone [D2], pimozide [D2]) as did two DA indirect agonists, amfonelic acid and nomifensine. The inhibitory effect of the agonists was not antagonized by the less active antagonists, SCH-23390 [D1] or spiperone [D2]. Taken together these results suggest that the inhibitory effects do not involve specific binding of DA or its agonists/antagonists to dopaminergic receptors mediating changes in cAMP concentration. This conclusion is also supported by the observation that addition of dibutyryl cAMP did not change brain AA. It appears more likely that DA and dopaminergic drugs inhibit AA by a direct effect on the enzyme, as suggested by the competitive nature of DA and SKF-38393 inhibition of AA (Ki's of 59 and 84 microM, respectively). The functional significance of this effect should still be demonstrated but this mechanism may represent an important physiological pathway through which neurotransmitters could rapidly affect steroid-dependent processes such as the neural synthesis of estrogens. This would provide a mean by which environmental stimuli could affect reproductive behavior and physiology.

摘要

在鹌鹑的视前区(POA),解剖学和药理学数据表明,儿茶酚胺可能参与睾酮(T)向雌激素的芳香化过程的调控。然而,介导这种酶活性调控的生化机制尚未得到探究。本研究旨在调查儿茶酚胺、多巴胺(DA)和去甲肾上腺素(NE)是否能够直接影响POA匀浆体外孵育过程中所测得的芳香化酶活性(AA)。通过测量[1β-3H]-雄烯二酮产生的氚化水,对成年雄性日本鹌鹑的POA-下丘脑的AA进行定量分析。酶活性与孵育时间和匀浆蛋白含量呈线性关系。它呈现出典型的米氏动力学,表观Km为2.8 nM,Vmax为266.6 fmol h(-1) mg湿重(-1)。然后在儿茶酚胺及其一些受体激动剂或拮抗剂存在的情况下,以25 nM的底物浓度,10(-3)和10(-6) M两种浓度测量AA。去甲肾上腺素和哌唑嗪(α1-肾上腺素能拮抗剂)在这两种浓度下对AA均无影响或影响非常有限。相比之下,多巴胺以及一些D1和/或D2受体激动剂(阿扑吗啡[D1/D2]、SKF-38393 [D1]和RU-24213 [D2])在10(-3) M浓度下可使AA降低40%至70%。一种D2受体拮抗剂也对AA产生了主要抑制作用(舒必利),而其他拮抗剂要么没有显著影响,要么仅使酶活性适度降低(SCH-23390 [D1]、螺哌隆[D2]、匹莫齐特[D2]),两种多巴胺间接激动剂氨苯磺酸和诺米芬辛也是如此。活性较低的拮抗剂SCH-23390 [D1]或螺哌隆[D2]并未拮抗激动剂的抑制作用。综合这些结果表明,抑制作用并不涉及多巴胺或其激动剂/拮抗剂与介导cAMP浓度变化的多巴胺能受体的特异性结合。这一结论也得到了如下观察结果的支持,即添加二丁酰cAMP并未改变脑AA。DA和多巴胺能药物似乎更有可能通过对该酶的直接作用来抑制AA,正如DA和SKF-38393对AA抑制作用的竞争性本质所表明的那样(Ki分别为59和84 microM)。这种作用的功能意义仍有待证实,但这种机制可能代表了一条重要的生理途径,通过该途径神经递质可以快速影响类固醇依赖性过程,如雌激素的神经合成。这将提供一种环境刺激可能影响生殖行为和生理的方式。

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