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鲨鱼γ-氨基丁酸-苯二氮䓬受体:苯二氮䓬受体并非很晚才在系统发育中出现的进一步证据。

The shark GABA-benzodiazepine receptor: further evidence for a not so late phylogenetic appearance of the benzodiazepine receptor.

作者信息

Hebebrand J, Friedl W, Reichelt R, Schmitz E, Möller P, Propping P

机构信息

Institut für Humangenetik der Universität Bonn, F.R.G.

出版信息

Brain Res. 1988 Apr 19;446(2):251-61. doi: 10.1016/0006-8993(88)90884-0.

Abstract

Whilst the brain-specific benzodiazepine receptor has been assumed to show a late evolutionary appearance, we present evidence for the presence of a central benzodiazepine binding site in sharks, which shows a high affinity for [3H]Ro 15-1788. However, the receptor density and the affinities of several benzodiazepine receptor ligands are lower than in mammals, thus presumably explaining why the benzodiazepine binding sites had previously escaped detection in elasmobranchs. Additionally, radio- and immunohistochemistry were performed to localize the radioligand binding sites and the antigenic sites of the shark gamma-aminobutyric acid (GABA)-benzodiazepine receptor. In cerebellum, the granular layer reveals a high density of [3H]muscimol binding sites. The immunoreaction obtained with the beta-subunit-specific monoclonal antibody bd-17 seemingly parallels the distribution of high-affinity GABA binding sites. In contrast, [3H]Ro 15-1788 binding sites are evenly distributed in the molecular and granular layers, thus the results are similar to those previously described for rat cerebellum. Apparently, the respective distributions in this brain region are well conserved throughout vertebrate evolution.

摘要

虽然脑特异性苯二氮䓬受体被认为在进化后期才出现,但我们提供证据表明鲨鱼体内存在中枢苯二氮䓬结合位点,该位点对[3H]Ro 15 - 1788表现出高亲和力。然而,该受体密度以及几种苯二氮䓬受体配体的亲和力低于哺乳动物,这大概解释了为何苯二氮䓬结合位点此前在板鳃亚纲动物中未被检测到。此外,进行了放射自显影和免疫组织化学以定位鲨鱼γ-氨基丁酸(GABA)-苯二氮䓬受体的放射性配体结合位点和抗原位点。在小脑,颗粒层显示出高密度的[3H]蝇蕈醇结合位点。用β亚基特异性单克隆抗体bd - 17获得的免疫反应似乎与高亲和力GABA结合位点的分布平行。相比之下,[3H]Ro 15 - 1788结合位点在分子层和颗粒层中均匀分布,因此结果与先前描述的大鼠小脑相似。显然,在整个脊椎动物进化过程中,该脑区的各自分布情况保存良好。

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