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阿片受体调制剂脑室内和腹腔内给药对雄性大鼠纳米和常规 ZnO 抗焦虑作用的影响。

Effect of Intra CA1 and Intraperitoneal Administration of Opioid Receptor Modulating Agents on The Anxiolytic Properties of Nano and Conventional ZnO in Male Rats.

机构信息

Department of Biology, Faculty of Sciences, Shahid Chamran University, Ahvaz, Iran.

Department of Pharmacology, Faculty of Veterinary Medicine, Shahid Chamran University, Ahvaz, Iran.

出版信息

Cell J. 2014 Summer;16(2):163-70. Epub 2014 May 25.

Abstract

OBJECTIVE

Nano components are today's new wonder material. However, the safety or toxicity of these components in humans is not yet clear. In a previous study we indicated that nano ZnO (nZnO) has a stronger anxiolytic effect compared to the conventional ZnO (cZnO). The present study was designed to evaluate the intraperitoneal administration of an opioidergic receptor agonist and antagonist of as well as the intra CA1 administration of an opioidergic receptor antagonist on the anxiolytic properties of nano and conventional ZnO in adult male Wistar rats.

MATERIALS AND METHODS

In this experimental study, rats received drugs via two modes of injection; intraperitoneal (IP.) and intra CA1 (intra hippocampus, CA1 area). Firstly, nZnO (5, 10, 20 mg/kg), cZnO (5, 10, 20 mg/kg), morphine 6 mg/kg, and naloxone 1 mg/kg were injected IP and naloxone 1µg/rat was injected intra CA1. Subsequently, morphine and na- loxone (IP and intra CA1) were co-injected with the effective dose of nZnO and cZnO. An elevated plus maze was used to evaluate anxiety related behavior and anxiety parameters 30 minutes after the second injection.

RESULTS

The results indicated that the anxiolytic effects of nZnO 5 mg/kg and cZnO 10 mg/kg were equal. When injected intraperitoneally, naloxone increased anxiety but did not inhibit the anxiolytic effect of nZnO and cZnO. The anxiolytic effects of morphine potentiated the anxio- lytic effects of ZnO, particularly nZno. When introduced via intra CA1 injection naloxone alone had no effect on anxiety behaviors and did not inhibit the anxiolytic effect of nZnO.

CONCLUSION

It seems that the opioidergic system activity involved in the anxiolytic effect of nano and conventional ZnO may operate through shared and unshared pathways.

摘要

目的

纳米成分是当今的新型神奇材料。然而,这些成分在人类中的安全性或毒性尚不清楚。在之前的一项研究中,我们表明纳米氧化锌(nZnO)比传统氧化锌(cZnO)具有更强的抗焦虑作用。本研究旨在评估阿片受体激动剂和拮抗剂的腹腔内给药以及阿片受体拮抗剂在成年雄性 Wistar 大鼠中纳米和常规 ZnO 的抗焦虑特性中的 CA1 内给药。

材料和方法

在这项实验研究中,大鼠通过两种注射方式接受药物;腹腔内(IP.)和 CA1 内(海马 CA1 区)。首先,nZnO(5、10、20mg/kg)、cZnO(5、10、20mg/kg)、吗啡 6mg/kg 和纳洛酮 1mg/kg 被注射到 IP 中,纳洛酮 1µg/大鼠被注射到 CA1 内。随后,将吗啡和纳洛酮(IP 和 CA1 内)与 nZnO 和 cZnO 的有效剂量共同注射。高架十字迷宫用于评估第二次注射 30 分钟后的焦虑相关行为和焦虑参数。

结果

结果表明,nZnO 5mg/kg 和 cZnO 10mg/kg 的抗焦虑作用相等。腹腔内注射时,纳洛酮增加焦虑,但不抑制 nZnO 和 cZnO 的抗焦虑作用。吗啡的抗焦虑作用增强了 ZnO 的抗焦虑作用,特别是 nZno。当通过 CA1 内注射引入时,纳洛酮单独对焦虑行为没有影响,也不抑制 nZnO 的抗焦虑作用。

结论

似乎纳米和常规 ZnO 的抗焦虑作用涉及阿片受体系统活动,可能通过共享和非共享途径进行。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/20e8/4071981/f8cf2bafcf50/Cell-J-16-163-g01.jpg

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