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神经甾体在胎鼠前脑GABAA受体上的作用

Neurosteroid action at the GABAA receptor in fetal rat forebrain.

作者信息

Kellogg C K, Olson V G, Pleger G L

机构信息

Department of Brain and Cognitive Sciences, University of Rochester, NY 14627, USA.

出版信息

Brain Res Dev Brain Res. 1998 Jun 15;108(1-2):131-7. doi: 10.1016/s0165-3806(98)00042-x.

DOI:10.1016/s0165-3806(98)00042-x
PMID:9693791
Abstract

In utero exposure to diazepam (DZ), a positive modulator of the GABAA (gamma-aminobutyric acid type A) receptor exerts profound effects on the offspring that become most apparent after the maturation of the brain during puberty and that are often sex specific, suggesting that the early exposure might have interfered with organizing actions of sex steroids. In addition to genomic actions, many reduced steroids interact directly with membrane receptors, including the GABAA receptor. In the present study, the effect of in vitro exposure to neurosteroids on GABA-stimulated 36chloride uptake in synaptoneurosomes from adult cerebral cortex or fetal forebrain (gestation day 20) was examined. The initial study examined the effects of incubation with DZ (10 microM) and the neuroactive steroid, 3 alpha,5 beta-THP (500 nM), alone and in combination. In adult tissue, the presence of either drug alone decreased the EC50 for GABA stimulation, and incubation with both drugs had an additive effect. In fetal tissue, while both compounds decreased the EC50, an additive effect was apparent only when comparing the combined exposure to 3 alpha,5 beta-THP alone. DZ alone reduced the EC50 as much as both drugs together. In the second study, the effect of in vitro exposure to androsterone (2.5 microM) was evaluated in male and female fetal tissue separately as well as in the adult. Androsterone enhanced the sensitivity to GABA in all groups but also reduced the efficacy of GABA in fetal tissue, irrespective of gender. While neurosteroids and DZ elicited similar responses in fetal and adult tissue, the study identified a greater vulnerability of fetal GABAA receptors to modulatory compounds.

摘要

子宫内暴露于地西泮(DZ),一种γ-氨基丁酸A型(GABAA)受体的正向调节剂,会对后代产生深远影响,这些影响在青春期大脑成熟后最为明显,且通常具有性别特异性,这表明早期暴露可能干扰了性类固醇的组织作用。除了基因组作用外,许多还原型类固醇还直接与膜受体相互作用,包括GABAA受体。在本研究中,检测了体外暴露于神经甾体对成年大脑皮质或胎儿前脑(妊娠第20天)突触体中GABA刺激的氯离子摄取的影响。初步研究检测了单独及联合孵育DZ(10微摩尔)和神经活性甾体3α,5β-四氢孕酮(500纳摩尔)的效果。在成年组织中,单独使用任何一种药物都会降低GABA刺激的半数有效浓度(EC50),同时使用两种药物具有相加作用。在胎儿组织中,虽然两种化合物都降低了EC50,但只有在将联合暴露与单独使用3α,5β-四氢孕酮进行比较时,相加作用才明显。单独使用DZ降低EC50的程度与两种药物一起使用时相同。在第二项研究中,分别评估了体外暴露于雄甾酮(2.5微摩尔)对雄性和雌性胎儿组织以及成年组织的影响。雄甾酮增强了所有组对GABA的敏感性,但也降低了胎儿组织中GABA的效能,与性别无关。虽然神经甾体和DZ在胎儿和成年组织中引发了相似的反应,但该研究发现胎儿GABAA受体对调节化合物更敏感。

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