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利用肽类催产素和血管加压素受体配体在大鼠高架十字迷宫中调节焦虑行为。

Modulation of anxiety behavior in the elevated plus maze using peptidic oxytocin and vasopressin receptor ligands in the rat.

机构信息

School of Psychology and Psychiatry, Monash University, Clayton VIC, Australia.

出版信息

J Psychopharmacol. 2012 Apr;26(4):532-42. doi: 10.1177/0269881111416687. Epub 2011 Sep 2.

DOI:10.1177/0269881111416687
PMID:21890582
Abstract

Oxytocin (OT) and arginine vasopressin (AVP), in their capacities as neuromodulators, are believed to play an important role in mood control, including regulation of the anxiety response. In the present study, the contributions of oxytocin and vasopressin receptor modulation to anxiety-like behaviors were examined in male Sprague-Dawley rats. The behavioral effects of the OT receptor agonist, carbetocin (intracerebroventricular, intravenous and intraperitoneal routes), the AVP receptor agonist desmopressin (intravenous route), and the OT/AVP(1A) receptor antagonist atosiban (intravenous route) were evaluated in the elevated plus maze. The benzodiazepine diazepam was included as a positive control. Central but not systemic administration of carbetocin produced pronounced anxiolytic-like behavioral changes comparable to those measured following systemic diazepam treatment. The anxiolytic efficacy of carbetocin was maintained following 10 days of once-daily treatment, contrasting with the effects of diazepam which were no longer distinguishable from saline treatment. Systemic administration of desmopressin produced anxiogenic-like effects whereas systemic atosiban produced anxiolytic-like effects. Co-administration of desmopressin with atosiban resulted in saline-like behavioral responses, implicating an AVP(1A) receptor mechanism in the anxiolytic and anxiogenic effects of these neuropeptides following systemic administration. A peripherally-mediated antidiuretic effect of desmopressin on water consumption was also demonstrated. These results highlight the potential therapeutic utility of AVP(1A) receptor blockade in the modulation of anxiety-related behaviors; AVP(1A) receptor blockade appears to be a more promising pharmacological target than does OT receptor activation following systemic drug administration.

摘要

催产素(OT)和精氨酸加压素(AVP)作为神经调质,被认为在情绪控制中发挥重要作用,包括调节焦虑反应。在本研究中,研究了 OT 和血管加压素受体调节对雄性 Sprague-Dawley 大鼠焦虑样行为的影响。通过高架十字迷宫评估了 OT 受体激动剂卡贝缩宫素(脑室内、静脉内和腹腔内途径)、AVP 受体激动剂去氨加压素(静脉内途径)和 OT/AVP(1A)受体拮抗剂阿托西班(静脉内途径)的行为效应。地西泮被包括作为阳性对照。卡贝缩宫素的中枢而非全身给药产生了明显的抗焦虑样行为变化,与全身地西泮治疗后测量的变化相当。卡贝缩宫素的抗焦虑功效在每天一次的 10 天治疗后得以维持,与地西泮的作用形成对比,后者与盐水治疗无明显区别。去氨加压素的全身给药产生了焦虑样效应,而阿托西班的全身给药产生了抗焦虑样效应。去氨加压素与阿托西班共同给药导致行为反应类似于盐水,这表明在全身给予这些神经肽后,AVP(1A)受体机制参与了它们的抗焦虑和焦虑作用。还证明了去氨加压素对水消耗的外周介导的抗利尿作用。这些结果强调了 AVP(1A)受体阻断在调节焦虑相关行为中的潜在治疗效用;AVP(1A)受体阻断似乎是比全身给药后 OT 受体激活更有前途的药理学靶点。

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