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痛敏肽/孤啡肽FQ肽拮抗剂J-113397减轻大鼠因接触捕食者而产生的不良行为影响。

Mitigation of adverse behavioral impact from predator exposure by the nociceptin/orphanin FQ peptide antagonist J-113397 in rats.

作者信息

Genovese Raymond F, Dobre Stefania

机构信息

Center for Military Psychiatry and Neuroscience, Walter Reed Army Institute of Research, Silver Spring, Maryland, USA.

出版信息

Behav Pharmacol. 2017 Oct;28(7):521-530. doi: 10.1097/FBP.0000000000000329.

Abstract

The nociceptin/orphanin FQ peptide (NOP) receptor is believed to have an integral modulatory function in the stress response system. We evaluated the highly selective NOP antagonist J-113397 (7.5 and 20.0 mg/kg), using a predator exposure in which rats were exposed to predator cats as a stressor. A single dose of J-113397 or vehicle was administered (intraperitoneally) shortly before exposure to the predators or a sham exposure. Behavioral impact was measured using elevated plus maze (EPM), open field activity (OFA), and an olfactory discrimination (OD). The predator exposure produced a relatively long-lasting deficit (decreased time in open arms, decreased basic activity) on the EPM while having little effect on performance on the OFA or OD. J-113397 mitigated the performance deficits on the EPM in a dose-dependent manner while having little effect on performance on the OFA or OD. The largest dose of J-113397, administered with a sham exposure, was essentially devoid of effects on the EPM, OFA, and OD. These results demonstrate that J-113397 can significantly and selectively mitigate the effects of a stressor typically used in a preclinical model of post-traumatic stress disorder. Furthermore, these results are consistent with and extend previous results showing that the NOP receptor has an important role in the response to stress and that NOP antagonism may, potentially, have therapeutic benefit in stress disorders.

摘要

痛敏肽/孤啡肽FQ肽(NOP)受体被认为在应激反应系统中具有不可或缺的调节功能。我们使用捕食者暴露实验来评估高选择性NOP拮抗剂J-113397(7.5和20.0毫克/千克),在该实验中,将大鼠暴露于捕食者猫作为应激源。在暴露于捕食者或假暴露之前不久(腹腔内)给予单剂量的J-113397或赋形剂。使用高架十字迷宫(EPM)、旷场活动(OFA)和嗅觉辨别(OD)来测量行为影响。捕食者暴露在EPM上产生了相对持久的缺陷(开放臂停留时间减少、基础活动减少),而对OFA或OD的表现影响很小。J-113397以剂量依赖的方式减轻了EPM上的表现缺陷,而对OFA或OD的表现影响很小。与假暴露一起给予的最大剂量的J-113397对EPM、OFA和OD基本没有影响。这些结果表明,J-113397可以显著且选择性地减轻创伤后应激障碍临床前模型中通常使用的应激源的影响。此外,这些结果与先前的结果一致并有所扩展,表明NOP受体在应激反应中具有重要作用,并且NOP拮抗作用可能在应激障碍中具有治疗益处。

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