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胸腺五肽可拮抗应激诱导的γ-氨基丁酸/苯二氮䓬受体复合物的变化。

Thymopentin antagonizes stress-induced changes of GABA/benzodiazepine receptor complex.

作者信息

Klusa V, Kiivet R A, Muceniece R, Liepa I, Harro J, Svirskis S, Andermanis A, Rägo L

机构信息

Department of Pharmacology, Tartu University, Estonia.

出版信息

Regul Pept. 1990 Mar 5;27(3):355-65. doi: 10.1016/0167-0115(90)90124-f.

Abstract

Intraperitoneal administration of thymopentin, a thymopentin II-derived pentapeptide, had no stable and evident effect in the two anxiety models (elevated plus-maze and licking-conflict test) studied. However, in the elevated plus-maze test thymopentin antagonized the behavioral effects of DMCM, a beta-carboline derivative with anxiogenic properties. Further, it was demonstrated that the licking-conflict test procedure itself produced a significant elevation of plasma corticosterone levels, increased the number of [3H]flunitrazepam and decreased the number of [3H]muscimol binding sites in rat hippocampus. The forced-swimming stress similarly to the licking-conflict test also caused an increase in hippocampal [3H]flunitrazepam binding sites. Although ineffective behaviorally in the tests for anxiety, thymopentin pretreatment effectively reversed the changes in corticosterone levels caused by the licking-conflict test. Moreover, it normalized the changed number of benzodiazepine and GABA receptors after stressful stimuli. It is well known that not all anxiolytic drugs (i.e. buspirone) are equally active in behavioral tests for anxiety. According to our data we propose that thymopentin has stress-protective activity. As in vivo and in vitro thymopentin did not change [3H]-flunitrazepam and [3H]muscimol binding, the direct effect of this peptide on the GABA-benzodiazepine-Cl- ionophore receptor complex is unlikely. The action of this peptide on GABA release and/or metabolism can be suggested.

摘要

在研究的两种焦虑模型(高架十字迷宫和舔舐冲突试验)中,腹腔注射胸腺五肽(一种源自胸腺五肽II的五肽)没有稳定且明显的效果。然而,在高架十字迷宫试验中,胸腺五肽拮抗了DMCM(一种具有致焦虑特性的β-咔啉衍生物)的行为效应。此外,研究表明舔舐冲突试验本身会使大鼠血浆皮质酮水平显著升高,增加海马体中[3H]氟硝西泮结合位点的数量,并减少[3H]蝇蕈醇结合位点的数量。与舔舐冲突试验类似,强迫游泳应激也会导致海马体中[3H]氟硝西泮结合位点增加。尽管胸腺五肽在焦虑试验中行为学上无效,但预处理能有效逆转舔舐冲突试验引起的皮质酮水平变化。此外,它还能使应激刺激后苯二氮䓬和GABA受体数量的改变恢复正常。众所周知,并非所有抗焦虑药物(如丁螺环酮)在焦虑行为试验中的活性都相同。根据我们的数据,我们认为胸腺五肽具有应激保护活性。由于体内和体外试验中胸腺五肽均未改变[3H] - 氟硝西泮和[3H]蝇蕈醇的结合,因此该肽对GABA - 苯二氮䓬 - Cl⁻离子载体受体复合物的直接作用不太可能。可以推测该肽对GABA释放和/或代谢有作用。

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